Method compositions and apparatus for treating and preventing respiratory viral infections

ABSTRACT

Respiratory viral infections may be effectively prevented or treated by administering an aerosol spray comprising a polyoxometalate to the lungs.

This invention was made with the assistance of U.S. Government funding under NIH Grant No. AI 32903. The U.S. Government may have some rights in this invention.

This application is a Division of application Ser. No. 08/399,700 filed Mar. 3, 1995 and now U.S. Pat. No. 5,824,706, which is a continuation-in-part of application Ser. No. 08/312,561, filed Sep. 26, 1994, abandoned.

BACKGROUND OF THE INVENTION

1. Field of the Invention

The present invention relates to a method of treating respiratory viral infections, compositions useful for treating and/or preventing respiratory viral infections, and apparatus for delivering such compositions. The present invention also relates to methods of treating herpesvirus infection and hepadnavirus infection.

2. Discussion of the Background

Respiratory viral infections are an important cause of respiratory disease. Examples of such respiratory diseases arising from viral infection include influenza A, influenza B, and respiratory syncytial virus (RSV).

There are a number of drugs available for such respiratory viral infections, including ribavirin, amantadine, and rimantadine. However, none of these therapies are completely satisfactory. In particular, such drugs may be accompanied by side effects including nausea, hematological toxicity, and the development of resistant viruses.

Polyoxometalates are soluble inorganic cluster-like compounds formed principally of oxide anion and early transition metal cations. Some major polyoxometalate structural families are as follows: (1) the Keggin class (e.g., α-SiW₁₂ O₄₀ ⁴⁻); (2) the Wells-Dawson class (e.g., P₂ W₁₈ O₆₂ ⁶⁻); (3) fragments from these structures (e.g., PW₁₁ O₃₉ ⁷⁻); (4) the Keggin derived sandwich compounds (e.g., K₁₀ Fe₄ (H₂ O)₂ (PW₉ O₃₄)₂, code name, HS058); (5) the hexametalates or the Lindquist class (e.g., W₆ O₁₉ ²⁻), decatungstate (W₁₀ O₃₂ ⁴⁻); and (6) the Preyssler ion [(NaP₅ W₃₀ O₁₁₄)¹⁴⁻ ] (Hill, C. L., et al, J. Med. Chem, vol. 33, pp. 2767-2772 (1990); Hill, C. L., et al, in Advances in Chemotherapy of AIDS, Diasio, R. B., et al, Eds, Pergamon Press, New York, pp. 33-41 (1990).

The potent and selective anti-human immunodeficiency virus type-1 (HIV-1) activity of polyoxometalates in infected human peripheral mononuclear (PBM) cells or cultured CD4+ T-cell lines has been reported by several workers. (Hill, C. L., et al, J. Med. Chem, vol. 33, pp. 2767-2772 (1990); Hill, C. L., et al, in Advances in Chemotherapy of AIDS, Diasio, R. B., et al, Eds, Pergamon Press, New York, pp. 33-41 (1990); Kim, G.-S., et al, J. Med. Chem., vol. 37 (1994), Yamamoto, N. et al, Mol. Pharmacol., vol. 42, pp. 1109-1117 (1992). Polyoxometalates have also been shown to be broadly inhibitory against retro-, myxo-, herpes-, toga-, rhabdo- and arenaviruses replications in vitro (Ikeda S. et al, Antiviral Chem. Chemother., vol. 4, pp. 253-262 (1993); Yamamoto, N. et al, Mol. Pharmacol., vol. 42, pp. 1109-1117 (1992). The mechanism of anti-HIV action may be attributed to inhibition of virus cell binding and inhibition of syncytium formation (Hill, C. L., et al, J. Med. Chem, vol. 33, pp. 2767-2772 (1990); Kim, G.-S. et al, Unpublished work; Take, Y., et al, Antiviral Res., vol. 15, pp. 113-124 (1991). A similar mechanism of antiviral action has also been suggested against influenza virus (FluV)-A and respiratory syncytial virus (RSV) (Ikeda S. et al, Antiviral Chem. Chemother., vol. 4, pp. 253-262 (1993).

However, to date, there is no report of the treatment of respiratory viral infection by the administration of a polyoxometalate. Thus, there remains a need for a method of treating respiratory viral infections. There also remains a need for compositions and apparatus useful for treating respiratory viral infections. There also remains a need for treating human herpesvirus infections and hepadnavirus infections.

SUMMARY OF THE INVENTION

Accordingly, it is one object of the present invention to provide novel methods for treating respiratory viral infections.

It is another object of the present invention to provide novel methods for preventing respiratory viral infections.

It is another object of the present invention to provide novel compositions for treating respiratory viral infections.

It is another object of the present invention to provide novel compositions for preventing respiratory viral infections.

It is another object of the present invention to provide apparatus for dispensing such compositions.

It is another object of the present invention to provide novel methods for treating human herpesvirus infection.

It is another object of the present invention to provide novel methods for treating human hepadnavirus infection.

These and other objects, which will become apparent during the following detailed description, have been achieved by the inventors' discovery that administration of an effective amount of polyoxometalate is effective for the treatment and prevention of respiratory viral infection and that polyoxometalates may be conveniently administered to the lungs of an animal in the form of an aerosol spray. The inventors have also discovered that human herpesvirus infection and human hepadnavirus infection may be effectively treated by administering an effective amount of a polyoxometalate.

BRIEF DESCRIPTION OF THE DRAWINGS

A more complete appreciation of the invention and many of the attendant advantages thereof will be readily obtained as the same becomes better understood by reference to the following detailed description when considered in connection with the accompanying drawings, wherein:

FIGS. 1a and b show the inhibitory effects of HS-058 on virus yield in MDCK cells infected with FluV-A. Cells were infected with a multiplicity of infection (moi) of 5.0 (FIG. 1a), or 0.005 (FIG. 1b). cultures were treated with 4.4 EC₅₀ (6.0 μM) of HS-058 from 60 min before (Δ) or 90 min after (□) virus inoculation to the end of the experiment at 35° C. Control (, mock treated) and experimental cultures were incubated at 37° C. for 90 min after virus inoculation, washed 3 times with maintenance medium, and then incubated at 35° C. with or without compound in medium; and

FIG. 2 shows the inhibitory effect of HS-058 against antigen synthesis and syncytium formation of RSV in HeLa cell monolayers. HeLa cells in Lab-Tec chamber were infected with 100 PFU/well of RSV and incubated at 37° C. After virus adsorption to cells by incubation for 90 min, infected cultures were treated with 1.6, 6, and 25 μM of HS-058 at 35° C. At 48 hr after infection, cells were fixed with acetone and stained with anti-RSV rabbit serum conjugated with fluorescein isothiocyanate. Cells were observed under a fluorescent microscope, and the number of antigen positive cells per 10 microscopic fields () and number of infected cells in one syncytium (∘) were counted.

DETAILED DESCRIPTION OF THE PREFERRED EMBODIMENTS

Thus, in a first embodiment, the present invention provides a method for treating respiratory viral infections by administering an effective amount of a polyoxometalate. In the context of the present invention, the term polyoxometalate includes compounds of the formulae:

    ______________________________________                                         (BW.sub.12 O.sub.40).sup.5-                                                                            (I)                                                      (W.sub.10 O.sub.32).sup.4- (II)                                                (P.sub.2 W.sub.18 O.sub.62).sup.6- (III)                                       PW.sub.11 O.sub.39.sup.7- (IV)                                                 SiW.sub.11 O.sub.39.sup.8- (V)                                                 HSiW.sub.9 O.sub.34.sup.9- (VI)                                                HPW.sub.9 O.sub.34.sup.8- (VII)                                                (TM).sub.4 (PW.sub.9 O.sub.34).sub.2.sup.t- (VIII)                             (TM).sub.4 (P.sub.2 W.sub.15 O.sub.56).sub.2.sup.t- (IX)                       [NaP.sub.5 W.sub.30 O.sub.110 ].sup.14- (X)                                    (TM).sub.3 (PW.sub.9 O.sub.34).sub.2.sup.12- (XI)                              P.sub.2 W.sub.18 O.sub.6.sup.6- (XII)                                        ______________________________________                                    

wherein TM is a divalent or trivalent transition metal ion, such as Mn⁺², Fe⁺², Fe⁺³, Co⁺², Co⁺³, Ni⁺², Cu⁺² and Zn⁺², and wherein t is the valence of the anion which varies with the valency of TM;

    [A.sub.x W.sub.y Nb.sub.a O.sub.b ].sup.z-                 (XII)

in which A is one or more element selected from P, Si or Ge and x is zero or an integer from 1 to 40,

y is an integer from 1 to 10,

a is an integer from 1 to 8,

b is an integer from 15 to 150, and

z is an integer dependent upon the nature and oxidation state of element A,

and their aqua complexes and active fragments.

In the context of the anions of formula (XIV),preferred ions are those in which element A is selected from one or more of H, P, Ge and Si. Preferably, when x=0, y=6-a, a is an integer from 1 to 5 and b=19; when A=Si or Ge, x=2, y=18, a=6 and b=77, and when A=P, x=2 or 4, y=12, 15, 17 or 30, a=1, 3 or 6 and b=62 or 123. The skilled artisan will readily appreciate that a molecule/ionic structure does not exist for every value of each integer in the above formula; examples of active ingredients will be given hereafter.

Obviously, these anions will be administered in the form of a pharmaceutically acceptable salt containing one or more cations. The identity of the cation or cations is not particularly limited. Examples of suitable cations include H⁺, K⁺, Na⁺, NH₄ ⁺, mono-, di-, tri, or tetra-(C₁₋₄)-alkylammonium, mono, di, tri, or tetra-(C₂₋₄)-alkanolammonium, monocationic naturally-occurring amino acids (such as histidinium, argininium, or lysinium), oligo- or polypeptides containing one or more protonated basic amino acid residues, or any other common mono- or dication.

Specific examples of the polyoxometalates which may be used in the present invention are given in Table 1.

                                      TABLE 1                                      __________________________________________________________________________     CODE NUMBERS AND CHEMICAL FORMULAE OF POLYOXOMETALATES                                                        STRUCTURAL                                        CODE NUMBER FORMULAE FAMILY                                                  __________________________________________________________________________     HS-003  [(NMP).sub.2 H].sub.3 PW.sub.12 O.sub.40.sup.a                           HS-004 [(DMA).sub.2 H].sub.3 PMo.sub.12 O.sub.40.sup.b                         HS-005 (HPA-23) (NH.sub.4).sub.17 Na[NaSb.sub.9 W.sub.21 O.sub.86 ]                                         Inorganic Cryptate                                HS-006 a- and b-H.sub.5 BW.sub.12 O.sub.40 (BT)                                HS-007 a- and b-H.sub.6 ZnW.sub.12 O.sub.40                                    HS-009 a- and b-H.sub.6 P.sub.2 W.sub.18 O.sub.62                              HS-010 α-(NH.sub.4).sub.6 P.sub.2 W.sub.18 O.sub.62 Wells Dawson                                       HS-011 K.sub.10 Cu.sub.4 (H.sub.2                                             O).sub.2 (PW.sub.9 O.sub.34).sub.2.20H.sub.                                    2 O                                               HS-012 K.sub.10 Co.sub.4 (H.sub.2 O).sub.2 (PW.sub.9 O.sub.34).sub.2.20H                                    .sub.2 O                                          HS-013 Na.sub.7 PW.sub.11 O.sub.39                                             HS-013A Na.sub.7 PW.sub.11 O.sub.39.20H.sub.2 O + 2 C.sub.6 H.sub.5                                         P(O)(OH).sub.2                                    HS-014 (n-Bu.sub.4 N).sub.4 H.sub.3 PW.sub.11 O.sub.39                         HS-015 b-Na.sub.8 HPW.sub.9 O.sub.34                                           HS-016 (n-Bu.sub.4 N).sub.3 PMoW.sub.11 O.sub.39                               HS-017 a-[(nBu).sub.4 N].sub.4 Mo.sub.8 O.sub.26                               HS-018 (n-Bu.sub.4 N).sub.2 W.sub.6 O.sub.19                                   HS-019 (n-Bu.sub.4 N).sub.2 Mo.sub.6 O.sub.19                                  HS-020 a-(NH.sub.4).sub.n H.sub.(4-n) SiW.sub.12 O.sub.40                      NS-021 a-(NH.sub.4).sub.n H.sub.(5-n) BW.sub.12 O.sub.40                       HS-022 a-K.sub.5 BW.sub.12 O.sub.40                                            HS-023 K.sub.4 W.sub.4 O.sub.10 (O.sub.2)6                                     HS-024 b-Na.sub.9 HSiW.sub.9 O.sub.34                                          HS-025 Na.sub.6 H.sub.2 W.sub.12 O.sub.40                                      HS-026 (NH.sub.4).sub.14 [NaP.sub.5 W.sub.30 O.sub.110 ] Preyssler                                           HS-027 a-(NH.sub.4).sub.5 BW.sub.12                                           O.sub.40                                          HS-028 a-Na.sub.5 BW.sub.12 O.sub.40                                           HS-029 (NH.sub.4).sub.4 W.sub.10 O.sub.32                                      HS-030 (Me.sub.4 N).sub.4 W.sub.10 O.sub.32                                    HS-031 (HISH.sup.+).sub.n H.sub.(5-n) BW.sub.12 O.sub.40.sup.c                 HS-032 (LYSH.sup.+).sub.n H.sub.(5-n) BW.sub.12 O.sub.40.sup.d                 HS-033 (ARGH.sup.+).sub.n H.sub.(5-n) BW.sub.12 O.sub.40.sup.c                 HS-034 (HISH.sup.+).sub.n H.sub.(4-n) SiW.sub.12 O.sub.40                      HS-035 (LYSH.sup.+).sub.n H.sub.(4-n) SiW.sub.12 O.sub.40                      HS-036 (ARGH.sup.+).sub.n H.sub.(4-n) SiW.sub.12 O.sub.40                      HS-037 a-K.sub.8 SiW.sub.11 O.sub.39                                           HS-037A a-K.sub.8 SiW.sub.11 O.sub.39                                          HS-038 K.sub.10 (H.sub.2 W.sub.12 O.sub.42)                                    HS-039 K.sub.12 Ni.sub.3 (II)(PW.sub.9 O.sub.34).sub.2.nH.sub.2 O                                            HS-040 (NH.sub.4).sub.10 Co.sub.4                                             (II)(PW.sub.9 O.sub.34).sub.2.nH.sub.2 O                                        HS-041 K.sub.12 Pd.sub.3 (II)(PW.sub.9                                        O.sub.34).sub.2.nH.sub.2 O                        HS-042 Na.sub.12 P.sub.2 W.sub.15 O.sub.56.18H.sub.2 O Lacunary                                             (Defect)                                          HS-043 Na.sub.16 Cu.sub.4 (H.sub.2 O).sub.2 (P.sub.2 W.sub.15 O.sub.56).                                    sub.2.nH.sub.2 O                                  HS-044 Na.sub.16 Zn.sub.4 (H.sub.2 O).sub.2 (P.sub.2 W.sub.15 O.sub.56).                                    sub.2.nH.sub.2 O                                  HS-045 Na.sub.16 Co.sub.4 (H.sub.2 O).sub.2 (P.sub.2 W.sub.15 O.sub.56).                                    sub.2.nH.sub.2 O                                  HS-052 Na.sub.16 Ni.sub.4 (H.sub.2 O).sub.2 (P.sub.2 W.sub.15 O.sub.56).                                    sub.2.nH.sub.2 O Wells-Dawson Sandwich                                          HS-053 Na.sub.16 Mn.sub.4 (H.sub.2                                            O).sub.2 (P.sub.2 W.sub.15 O.sub.56).sub.2.                                    nH.sub.2 O Wells-Dawson Sandwich                  HS-054 Na.sub.16 Fe.sub.4 (H.sub.2 O).sub.2 (P.sub.2 W.sub.15 O.sub.56).                                    sub.2.nH.sub.2 O Wells-Dawson Sandwich                                          HS-055 K.sub.10 Zn.sub.4 (H.sub.2                                             O).sub.2 (PW.sub.9 O.sub.34).sub.2.20H.sub.                                    2 O Keggin Sandwich                               HS-056 K.sub.10 Ni.sub.4 (H.sub.2 O).sub.2 (PW.sub.9 O.sub.34).sub.2.nH.                                    sub.2 O Keggin Sandwich                           HS-057 K.sub.10 Mn.sub.4 (H.sub.2 O).sub.2 (PW.sub.9 O.sub.34).sub.2.nH.                                    sub.2 O Keggin Sandwich                           HS-058 K.sub.10 Fe.sub.4 (H.sub.2 O).sub.2 (PW.sub.9 O.sub.34).sub.2.nH.                                    sub.2 O Keggin Sandwich                           HS-059 K.sub.12 Cu.sub.3 (PW.sub.9 O.sub.34).sub.2.nH.sub.2 O                  HS-060 K.sub.12 (CoH.sub.2 O).sub.3 (PW.sub.9 O.sub.34).sub.2.nH.sub.2                                      O                                                 HS-061 K.sub.12 Zn.sub.3 (PW.sub.9 O.sub.34).sub.2.15H.sub.2 O                 HS-062 K.sub.12 Mn.sub.3 (PW.sub.9 O.sub.34).sub.2.15H.sub.2 O                 HS-063 K.sub.12 Fe.sub.3 (PW.sub.9 O.sub.34).sub.2.25H.sub.2 O                 HS-064 (ARGH.sup.+).sub.10 (NH.sub.4).sub.7 Na[NaSb.sub.9 W.sub.21                                          O.sub.86 ]                                        HS-065 (ARGH.sup.+).sub.5 HW.sub.11 O.sub.39.17H.sub.2 O                       HS-066 K.sub.7 Ti.sub.2 W.sub.10 O.sub.40                                      HS-067 [(CH.sub.3).sub.4 N].sub.7 Ti.sub.2 W.sub.10 O.sub.40                   HS-068 Cs.sub.7 Ti.sub.2 W.sub.10 O.sub.40                                     HS-069 [HISH.sup.+ ].sub.7 Ti.sub.2 W.sub.10 O.sub.40                          HS-070 (LYSH.sup.+).sub.n Na.sub.7-n PTi.sub.2 W.sub.10 O.sub.40                                             HS-071 (ARGH.sup.+).sub.n Na.sub.7-n                                          PTi.sub.2 W.sub.10 O.sub.40                       HS-072 Cs.sub.4 [SiW.sub.11 O.sub.39.O(SiCH.sub.2 CH.sub.2 C(O)OCH.sub.3                                    ).sub.2 ].sub.4 --                                HS-073 [TBA].sub.3 H.sub.3 V.sub.10 O.sub.28.sup.f                             HS-074 K.sub.7 HNb.sub.6 O.sub.19.13H.sub.2 O                                  HS-076 [(CH.sub.3).sub.4 N.sup.+ ].sub.4 SiW.sub.11 O.sub.39 --O(SiCH.su                                    b.2 CH.sub.2 C(O)OCH.sub.3).sub.2                 HS-077 [CH.sub.3).sub.4 N.sup.+ ].sub.4 PW.sub.11 O.sub.39 --(SiCH.sub.2                                     CH.sub.2 CH.sub.2 CN)                            HS-078 [(CH.sub.3).sub.4 N.sup.+ ].sub.4 PW.sub.11 O.sub.39 --(SiCH.sub.                                    2 CH.sub.2 CH.sub.2 Cl)                           HS-079 [(CH.sub.3).sub.4 N.sup.+ ].sub.4 PW.sub.11 O.sub.39 --(SiCH═                                    CH.sub.2)                                         HS-080 Cs.sub.4 [SiW.sub.11 O.sub.39 --(SiCH.sub.2 CH.sub.2 CH.sub.2                                        CN).sub.2 ]                                       HS-081 Cs.sub.4 [SiW.sub.11 O.sub.39 --(SiCH.sub.2 CH.sub.2 CH.sub.2                                        Cl).sub.2 ]                                       HS-082 Cs.sub.4 [SiW.sub.11 O.sub.39 --(SiCH═CH.sub.2).sub.2 ]                                           HS-083 [(CH.sub.3).sub.4 N.sup.+ ].sub.4                                      SiW.sub.11 O.sub.39 O(SiCH.sub.2 CH.sub.2                                      CH.sub.2 CH.sub.2 CH.sub.2 CH.sub.3).sub.2                                     Organic Derviatized                               HS-084 [(CH.sub.3).sub.4 N.sup.+ ].sub.4 SiW.sub.11 O.sub.39 --O(SiCH.su                                    b.2 CH.sub.2 CH.sub.2 Cl).sub.2                   HS-085 [(CH.sub.3).sub.4 N.sup.+ ].sub.4 SiW.sub.11 O.sub.39 --O(SiCH.su                                    b.2 CH.sub.2 CH.sub.2 CN).sub.2                   HS-086 [(CH.sub.3).sub.4 N.sup.+ ]SiW.sub.11 O.sub.39 --O(SiCH=CH.sub.2)                                    .sub.2                                            HS-087 [(CH.sub.2).sub.4 N.sup.+ ]SiW.sub.11 O.sub.39 --O(SiC(CH.sub.3)3                                    ).sub.2                                           HS-088 [(CH.sub.3).sub.4 N.sup.+ ]SiW.sub.11 O.sub.39 --O(SiCH.sub.2                                        CH(CH.sub.3).sub.2).sub.2                         HS-089 [(CH.sub.3).sub.4 N.sup.+ ].sub.3 PW.sub.11 O.sub.39 O(SiCH.sub.2                                     CH.sub.2 COOCH.sub.3).sub.2 Organic                                           Derivatized                                       HS-090 K.sub.5 Mn(II)PW.sub.11 O.sub.39 --nH.sub.2 O                           HS-091 K.sub.8 Mn(II)P.sub.2 W.sub.17 O.sub.61.nH.sub.2 O Transition                                        Metal Substituted                                   Polyoxmetalate                                                               HS-092 K.sub.6 Mn(II)SiW.sub.11 O.sub.39.nH.sub.2 O                            HS-093 K.sub.5 PW.sub.11 O.sub.39 (SiMe.sub.2).nH.sub.2 O                      HS-094 K.sub.3 PW.sub.11 O.sub.41 (PPh).sub.2.xH.sub.2 O                       HS-095 Na.sub.3 PW.sub.11 O.sub.41 (PPh).sub.2.xH.sub.2 O                      HS-096 K.sub.5 PTiW.sub.11 O.sub.40                                            HS-097 Cs.sub.5 PTiW.sub.11 O.sub.39                                           HS-098 K.sub.6 SiW.sub.11 O.sub.39 (SiMe.sub.2).nH.sub.2 O                     HS-099 K.sub.3 PW.sub.11 O.sub.41 (PFt).sub.2.nH.sub.2 O                       HS-100 KsiW.sub.11 O.sub.39 [SiPh(t-Bu)].nH.sub.2 O                            HS-101 K.sub.6 SiW.sub.11 O.sub.39 (SiPh.sub.2).nH.sub.2 O                     HS-102 K.sub.7 SiW.sub.9 Nb.sub.3 O.sub.40.nH.sub.2 O                          HS-103 Cs.sub.7 SiW.sub.9 Nb.sub.3 O.sub.40.nH.sub.2 O                         HS-104 Cs.sub.8 Si.sub.2 W.sub.18 Nb.sub.6 O.sub.77.nH.sub.2 O                 HS-105 (Me.sub.3 NH).sub.7 SiW.sub.9 Nb.sub.3 O.sub.40.nH.sub.2 O                                           Substituted Keggin                                HS-107 (CN.sub.3 H.sub.6).sub.7 SiW.sub.9 Nb.sub.3 O.sub.40.nH.sub.2 O                                       HS-108 (CN.sub.3 H.sub.6).sub.8 Si.sub.2                                      W.sub.18 Nb.sub.6 O.sub.77.nH.sub.2 O                                           HS-109 Rb.sub.7 SiW.sub.9 Nb.sub.3                                            O.sub.40.nH.sub.2 O                               HS-110 Rb.sub.8 Si.sub.2 W.sub.18 Nb.sub.6 O.sub.77.nH.sub.2 O                 HS-111 K8Si.sub.2 W.sub.18 Nb.sub.6 O.sub.77.nH.sub.2 O                        HS-112 K.sub.6 P.sub.2 Mo.sub.18 O.sub.62.nH.sub.2 O                           HS-113 (C.sub.5 H.sub.5 N).sub.7 HSi.sub.2 W.sub.18 Nb.sub.6 O.sub.77.nH                                    .sub.2 O                                          HS-114 (C.sub.5 H.sub.5 N).sub.7 SiW.sub.9 Nb.sub.3 O.sub.40.nH.sub.2 O        HS-115 (ARGH.sup.+).sub.8 SiW.sub.18 Nb.sub.6 O.sub.77.18H.sub.2 O                                           HS-116 (LYSH.sup.+).sub.7 KSiW.sub.18                                         Nb.sub.6 O.sub.77.18H.sub.2 O                     HS-117 (HISH.sup.+).sub.6 K.sub.2 SiW.sub.18 Nb.sub.6 O.sub.77.18H.sub.2                                     O                                                HS-118a H.sub.8 Si.sub.2 W.sub.18 Nb.sub.6 O.sub.77.nH.sub.2 O (2                                           batches)                                          HS-119 [(CH.sub.3).sub.4 N.sup.+ ].sub.4 SiW.sub.11 O.sub.39 --O(SiCH.su                                    b.2 CH.sub.3).sub.2                               HS-120 [(CH.sub.3).sub.4 N.sup.+ ].sub.4 SiW.sub.11 O.sub.39 --O(SiCH.su                                    b.3).sub.2                                        HS-121 [(CH.sub.3).sub.4 N.sup.+ ].sub.4 SiW.sub.11 O.sub.39 --O(SiC.sub                                    .16 H.sub.33).sub.2                               HS-122 Li.sub.7 HSi.sub.2 W.sub.18 Nb.sub.6 O.sub.77                           HS-123 Li.sub.9 P.sub.2 V.sub.3 Me.sub.3 W.sub.12 O.sub.62                     HS-124 Cs.sub.9 P.sub.2 V.sub.3 MeW.sub.12 O.sub.62                            HS-125 Cs.sub.12 P.sub.2 V.sub.3 W.sub.12 O.sub.62                             HS-126 K.sub.4 H.sub.2 PV.sub.4 W.sub.8 O.sub.40                               HS-127 Na.sub.12 P.sub.4 W.sub.14 O.sub.58                                     HS-128 Na.sub.14 H.sub.6 P.sub.6 W.sub.18 O.sub.79                             HS-129 a-K.sub.5 (NbO.sub.2)SiW.sub.11 O.sub.39                                HS-130 K.sub.5 (TaO.sub.2)SiW.sub.11 O.sub.39                                  HS-131 (Me.sub.3 NH).sub.5 (NbO.sub.2)SiW.sub.11 O.sub.39 Keggin Peroxo        HS-132 (Me.sub.3 NH).sub.5 NbSiW.sub.11 O.sub.40 Substituted Keggin                                          HS-133 (Me.sub.3 NH).sub.5 (TaO.sub.2)SiW.                                    sub.11 O.sub.39 Keggin Peroxo                     HS-134 K.sub.4 (NbO.sub.2)PW.sub.11 O.sub.39                                   HS-135 K.sub.7 (NbO.sub.2)P.sub.2 W.sub.12 O.sub.61                            HS-136 (Me.sub.3 NH).sub.7 (NbO.sub.2).sub.3 SiW.sub.9 O.sub.37 Keggin                                      Peroxo                                            HS-137 Cs.sub.7 (NbO.sub.2).sub.3 SiW.sub.9 O.sub.37                           HS-138 K.sub.6 (NbO.sub.2).sub.3 PW.sub.9 O.sub.37                             HS-139 Na.sub.10 (H.sub.2 W.sub.12 O.sub.42)                                   HS-140 K.sub.4 NbPW.sub.11 O.sub.40                                            HS-141 (Me.sub.3 NH).sub.4 NbPW.sub.11 O.sub.40                                HS-142 K.sub.5 NbSiW.sub.11 O.sub.40                                           HS-143 K.sub.5 TaSiW.sub.11 O.sub.40                                           HS-144 (Me.sub.3 NH).sub.5 TaSiW.sub.11 O.sub.40 Substituted Keggin                                          HS-145 K.sub.6 Nb.sub.3 PW.sub.9 O.sub.40        HS-146 K.sub.7 NbP.sub.2 W.sub.17 O.sub.62 Wells-Dawson                        HS-147 K.sub.7 (TiO.sub.2).sub.2 PW.sub.10 O.sub.38                            HS-148 K.sub.7 (TaO.sub.2).sub.3 SiW.sub.9 O.sub.37                            HS-149 K.sub.7 Ta.sub.3 SiW.sub.9 O.sub.40                                     HS-150 K.sub.6 (TaO.sub.2).sub.3 PW.sub.9 O.sub.37                             HS-151 K.sub.6 Ta.sub.3 PW.sub.9 O.sub.40                                      HS-152 K.sub.8 Co.sub.2 W.sub.11 O.sub.39                                      HS-153 H.sub.2 (Me.sub.4 N).sub.4 (EtSi).sub.2 C0W.sub.11 O.sub.40                                           HS-154 H.sub.2 (Me.sub.4 N).sub.4                                             (iso-C.sub.4 H.sub.9 Si).sub.2 CoW.sub.11                                      O.sub.40                                          HS-155 K.sub.9 (NbO.sub.2).sub.3 P.sub.2 W.sub.15 O.sub.59                     HS-156 K.sub.9 Nb.sub.3 P.sub.2 W.sub.15 O.sub.62                              HS-157 K.sub.12 (NbO.sub.2).sub.6 P.sub.2 W.sub.12 O.sub.56 Wells-Dawson                                     Peroxo                                           HS-158 K.sub.12 Nb.sub.6 P.sub.2 W.sub.12 O.sub.62 Wells-Dawson                                              HS-159 a.sub.2 -K.sub.10 P.sub.2 W.sub.17                                     O.sub.61                                          HS-160 K.sub.6 Fe(III)Nb.sub.3 P.sub.2 W.sub.15 O.sub.62                       HS-161 K.sub.7 Zn(II)Nb.sub.3 P.sub.2 W.sub.15 O.sub.62                        JM-1574 (NH.sub.4).sub.6 [a-P.sub.2 W.sub.18 O.sub.62).nH.sub.2 O                                            JM-1591 K.sub.12 [H.sub.2 P.sub.2                                             W.sub.12 O.sub.48 ].24H.sub.2 O                   JM-1591A K.sub.12 [H.sub.2 P.sub.2 W.sub.12 O.sub.48 ].24H.sub.2 O                                           JM-1605 K.sub.2 Na.sub.15 H.sub.45                                            (PtMo.sub.6 O.sub.24].8H.sub.2 O                  JM-1638 Ks[a.sub.2 -P.sub.2 W.sub.17 MoO.sub.62 ].nH.sub.2 O                   JM-1809A KHP.sub.2 V.sub.3 W.sub.15 O.sub.62.34H.sub.2 O                       JM-1819 K.sub.6 [P.sub.2 W.sub.12 Nb.sub.6 O.sub.62 ].24H.sub.2 O                                            JM-1827 Na.sub.6 [V.sub.10 O.sub.28                                           ].18H.sub.2 O                                     JM-1832 (Guanidinium).sub.8 H[PV.sub.14 O.sub.62 ].3H.sub.2 O                  JM-1835 K.sub.8 H[PV.sub.14 O.sub.62 ]                                         JM-1855 Na.sub.7 [MnV.sub.13 O.sub.38 ].18H.sub.2 O                            JM-2766 K.sub.6 [BW.sub.11 O.sub.39 Ga(OH.sub.2)].13H.sub.2 O                  JM-2768 K.sub.7 H[Nb.sub.6 O.sub.19 ].13H.sub.2 O                              JM-2768A K.sub.7 H[Nb.sub.6 O.sub.19 ].13H.sub.2 O                             JM-2775 [MeN/Na/K].sub.4 [Nb.sub.2 W.sub.4 O.sub.19 ]                          JM-2776 [Me.sub.4 N].sub.9 [P.sub.2 W.sub.15 Nb.sub.3 P.sub.62 ]                                             JM-2799 [Me.sub.4 N].sub.15 [HP.sub.4                                         W.sub.30 Nb.sub.6 O.sub.123 ].16H.sub.2 O                                       JM-2799A [Me.sub.4 N].sub.15 [HP.sub.4                                        W.sub.30 Nb.sub.6 O.sub.123 ].16H.sub.2 O                                       JM-2800 [Na/K].sub.6 Nb.sub.4 W.sub.2                                         O.sub.19 ]                                        JM-2801 [Me.sub.4 N/Na/K].sub.5 [Nb.sub.3 W.sub.3 O.sub.19 ].6H.sub.2 O        JM-2801A [Me.sub.4 N/Na/K].sub.5 [Nb.sub.3 W.sub.3 O.sub.19 ].6H.sub.2                                      O                                                 JM-2802 [Me.sub.5 CpPh).sub.4 V.sub.6 O.sub.19 ]                               JM-2815 K.sub.5 [CpTiSiW.sub.11 O.sub.39 ].12H.sub.2 O                         JM-2840 b.sub.2 -K.sub.8 [SiW.sub.11 O.sub.39 ].14H.sub.2 O                    JM-2841 a-K.sub.8 [SiW.sub.10 O.sub.36 ].12H.sub.2 O                           JM-2842 Cs.sub.7 Na.sub.2 [PW.sub.10 O.sub.37 ].8H.sub.2 O                     JM-2843 Cs.sub.6 [P.sub.2 W.sub.5 O.sub.23 ].7(1/2)H.sub.2 O                   JM-2844 g-Cs.sub.7 [PW.sub.10 O.sub.36 ].7H.sub.2 O                            JM-2869 K.sub.5 [SiNbW.sub.11 O.sub.40 ].7H.sub.2 O                            JM-2870 K.sub.4 [PNbW.sub.11 O.sub.40 ].12H.sub.2 O                            JM-2871 Na.sub.6 [Nb.sub.4 W.sub.2 O.sub.19 ].13H.sub.2 O                      JM-2871A Na.sub.6 [Nb.sub.4 W.sub.2 O.sub.19 ].20H.sub.2 O                     JM-2872 K.sub.6 [Nb.sub.4 W.sub.2 O.sub.19 ].7H.sub.2 O                        JM-2873 K.sub.4 [V.sub.2 W.sub.4 O.sub.19 ].3.5H.sub.2 O                       JM-2874 Na.sub.5 [V.sub.3 W.sub.3 O.sub.19 ].12H.sub.2 O                       JM-2875 K.sub.6 [PV.sub.3 W.sub.9 O.sub.40 ].14H.sub.2 O                       JM-2876 Na.sub.9 [A-b-GeW.sub.9 O.sub.34 ].8H.sub.2 O                          JM-2877 Na.sub.10 [A-a-GeW.sub.9 O.sub.34 ].9H.sub.2 O                         JM-2878 K.sub.7 [BV.sub.2 W.sub.10 O.sub.40 ].6H.sub.2 O                       JM-2879 Na.sub.5 [CH.sub.3 Sn(Nb.sub.6 O.sub.19)].10H.sub.2 O                  JM-2879A Na.sub.5 [CH.sub.3 Sn(Nb.sub.6 O.sub.19)].10H.sub.2 O                 JM-2881 Na.sub.8 [Pt(P(m-SO.sub.3 Ph).sub.3).sub.3 Cl].3H.sub.2 O                                            JM-2882 Na.sub.3 [P(m-SO.sub.3 Ph).sub.3                                      ].H.sub.2 O                                       JM-2919 (Me.sub.3 NH).sub.10 (H)[Si.sub.2 (ZrOH).sub.3 W.sub.18                                             O.sub.68 ].10H.sub.2 O                            JM-2919A (Me.sub.3 NH).sub.10 (H)[Si.sub.2 (ZrOH).sub.3 W.sub.18                                            O.sub.68 ].10H.sub.2 O                            JM-2921 K.sub.7 [A-a-GeNb.sub.3 W.sub.9 O.sub.40 ].18H.sub.2 O                 JM-2922 K.sub.7 [A-b-SiNb.sub.3 W.sub.9 O.sub.40 ].20H.sub.2 O                 JM-2923 (Me.sub.3 NH).sub.9 [A-a-HSi.sub.2 Nb.sub.6 W.sub.18 O.sub.78 ]        JM-2924 (Me.sub.3 NH).sub.9 [A-a-HGe.sub.2 Nb.sub.6 W.sub.18 O.sub.78 ]        JM-2925 (Me.sub.3 NH).sub.9 [A-a-HGe.sub.2 Nb.sub.6 W.sub.18 O.sub.78 ]        JM-2926 K.sub.7 (H)[A-a-Ge.sub.2 Nb.sub.6 W.sub.18 O.sub.77).18H.sub.2                                      O                                                 JM-2927 K.sub.8 [A-b-Si.sub.2 Nb.sub.6 W.sub.18 O.sub.77 ]                     JM-2928 (Me.sub.3 NH).sub.8 [A-b-Si.sub.2 Nb.sub.6 W.sub.18 O.sub.77         __________________________________________________________________________                                    ]                                                .sup.a NMP = Nmethylpyrrolidinone.                                             .sup.b DMA = N,NDimethylacetamide.                                             .sup.c HISH.sup.[30  = Histidinium                                             .sup.d LYSH.sup.+  = Lysinium                                                  .sup.e ARGH.sup.+  = Argininium                                                .sup.f TBA = Tetrabutylammonium                                          

Preferred polyoxometalates to be used in the present invention include HS-042, HS-053, HS-057, HS-058, HS-105, HS-106, HS-131, and HS-158. Particularly preferred are HS-058.

The present invention may be carried out by administering the polyoxomethalate directly to the lungs of the animal being treated. Preferably, the polyoxometalate is administered in the form of an aerosol.

The viral infections which may be treated by the present method include influenza A, influenza B, and RSV. Preferably, the present method is used to treat influenza A or RSV.

The present method may be used to treat respiratory viral infections in mammals such as humans, cats, horses, cows, pigs, sheep, monkeys, rabbits, rats, mice, etc., and birds such a chickens and turkeys.

Although the exact dosage of polyoxometalate to be administered will depend on the exact type, size, and condition of the animal being treated, the exact viral infection being treated, and the identity of the polyoxometalate being administered, good results are typically achieved with dosages of 0.1 to 100 mg/kg of body weight, preferably 1 to 30 mg/kg of body weight.

In certain circumstances, it may be preferred to coadminister the polyoxometalate with an additional active agent such as amantadine, rimantadine, or ribavivin. Of course, the present method may be carried out by administering a single polyoxometalate or a combination of two or more polyoxometalates.

In a preferred embodiment, the present invention provides a method for preventing respiratory viral infections. In this embodiment, the polyoxometalate is administered to a subject which has not been diagnosed as suffering from a respiratory viral infection but is considered to belong to an at risk population. With the exception of the subject to whom the polyoxometalate is administered this preventative embodiment is carried out as described above for the present method of treatment.

Examples of subjects in an at risk population to be administered polyoxometalate in the present method of prevention include subjects not yet suffering from a respiratory viral infection but in close contact with another individual, already diagnosed as suffering from a respiratory viral infection, such as a neonate or infant in a nursery in which at least one other neonate or infant has been diagnosed as suffering from a respiratory viral infection or a member of a barrack, nursing home, or school in which at least one other member has been diagnosed as suffering from a respiratory viral infection. Another at risk population is the elderly in general during flu season.

In another embodiment, the present invention provides pharmaceutical compositions which comprise a polyoxometalate for the treatment of a respiratory viral infection. Suitably, the compositions of the present invention are in a form which is conveniently administered as an aerosol spray.

The term aerosol includes compositions of matter in which particles or droplets are suspended or dispersed in a gaseous medium such a air. Thus, the term aerosol includes sprays. Apparatus and methods for forming aerosols are disclosed in Kirk-Othmer, Encyclopedia of Chemical Technology, 4th Ed., vol. 1, Wiley, New York, pp. 670-685 (1991) and Kirk-Othmer, Encyclopedia of Chemical Technology, 3rd. Ed., vol. 21, Wiley, New York, pp. 466-483 (1983), both of which are incorporated herein by reference.

The administration of the aerosol spray containing the polyoxometalate may be conveniently carried out by means of a delivery system capable of delivering an aerosol spray. Such delivery systems include conventional nasal aerosol spray bottles, or aerosol delivery via commonly used respiratory mechanical ventilation support equipment.

Typically, the present compositions will be in the form of an aqueous solution or dispersion of the polyoxometalate. The concentration of the polyoxometalate is suitably 0.1 μg/ml to 10 mg/ml, preferably 10 μg/ml to 1 mg/ml. The composition may further comprise a pH adjusting agent such as a physiologically tolerated acid or base, a buffer, or another active agent, such as ribavirin amantadine or rimantadine.

The present invention also provides dispensing devices for administering the present pharmaceutical compositions. Such dispensing devices comprise a container means which contains a pharmaceutical composition comprising the polyoxometalate and optionally another active ingredient; and means for forming an aerosol of the pharmaceutical composition. Suitable container means and suitable means for forming an aerosol are described in Kirk-Othmer, Encyclopedia of Chemical Technology, 4th Ed., vol. 1, Wiley, New York, pp. 670-685 (1991) and Kirk-Othmer, Encyclopedia of Chemical Technology, 3rd. Ed., vol. 21, Wiley, New York, pp. 466-483 (1983), both of which are incorporated herein by reference. Suitable container means include metal cans and glass and plastic bottles. Suitable means for forming an aerosol include combinations of propellants and valves (including an actuator and dip tube). A propellant may be present in the container under pressure, or the material in the container may be propelled by pressure created by mechanical force means such as, e.g., a bellows, bulb, or pump. Preferably, the present dispensing means is a pressurized aerosol can or an atomizer.

The present invention will no be described in more detail by referring to specific embodiments, which are not intended to be limiting.

Polyoxometalates have a broad spectrum of antimyxovirus activity. Several sulfates polysaccharides which have anionic charge inhibited adsorption of HIV, HSV, FluV-A and RSV, whereas they did not inhibit the adsorption of FluV-B, MLSV, SSPE, virus and PFluV-3 (Hosoya, M., et al, Antimicrob. Agents Chemother., vol. 35, pp. 2515-2520 (1991)). On the other hand, some polyoxometalates examined in this study had antiviral effects against FluV-A, RSV, MLSV, FluV-B, and PFluV-2. Inasmuch as the causative agents of viral respiratory infections are not rapidly identifiable by clinical diagnosis and there is a need for early treatment of patients to prevent the progress of infection, it is necessary to use a broad spectrum antiviral drug for the treatment of acute respiratory viral infections. From this point of view, HS-058 which shows a potent antiviral activity against FluV-A, FluV-B, RSV, MLSV, and PFluV-2 is especially preferred, because these viruses are the main causative agents of acute viral respiratory diseases (Hilleman, M. R., et al, J. Amer. Med. Assoc., vol. 180, pp. 444-453 (1962).

The structure-activity relationship of polyoxometalates and antimyxoviral activity was insightful. From our examination of 25 polyoxometalates against myxoviruses, 4 compounds emerged which showed potent and broad spectrum of antiviral activity. Among them, 2 compounds HS-054 and HS-058 are so-called "sandwich structures", HS-106 is a "double Keggin structure" and HS-158 is a hexasubstituted Wells-Dawson structure. HS-054 was apparently more potent in antiviral activity and less cytotoxic than its precursor complex (HS-042). The precursor complex of HS-058 and HS-106, HS-015 (PW₉ O₃₄ ⁹⁻), was not examined in this study for antimyxoviral activities but it was shown to be less effective against HIV-1 in a previous report (Hill, C. L., et al, J. Med. Chem, vol. 33, pp. 2767-2772 (1990)). The most effective compounds had Nb or Fe-base units (MO₆ octahedra, M=Nb or Fe) joining two halves of the molecule.

HS-058, one of the most active polyoxometalates did not inhibit the adsorption of FluV to MDCK cells and agglutination of chick erythrocytes by FluV-A, whereas it did inhibit hemolysis of chick erythrocytes after adsorption of virus at 4° C. as shown in Table 4, HS-058 did not inhibit FluV infection in MDCK cells when it was added at the time of virus adsorption (1 hour before to 1.5 hours after virus inoculation), whereas it did inhibit infection when it was present after virus adsorption for the whole course of the experiment (1 hour before to 120 hours after virus inoculation; FIG. 1 and Table 4). HS-058 was also inhibitory against FluV-A infection when it was added after virus adsorption to the end of culture (1.5 to 120 hours in Table 4). It is likely that polyoxometalates do not inhibit FluV adsorption to cellular membrane, but inhibit the fusion of the cleaved HA molecule and the cellular membrane. A similar result was reported using sulfated polysaccharides by Hosoya et al. (Hosoya, M., et al, Antimicrob. Agents Chemother., vol. 35, pp. 2515-2520 (1991)).

An insight on the mechanism of antiviral activity of HS-058 against FluV-A is apparent from the experiments on inhibition of virus replication in MDCK cells. When cells were infected with virus at a high moi and then treated with 4 EC₅₀ of HS-058, HS-058 had no effect on the yield of infectious Flu-V relative to control. However, when cells were infected with low moi of virus and then treated with HS-058, it inhibited virus yield relative to control. Clearly, HS-058 did not inhibit the growth of infectious virus in single cells, but inhibited the spread of virus from infected to uninfected cells.

HS-058 did not inhibit the antigen synthesis and plaque formation of RSV when it was added after the virus adsorption (Tables 4 and 5, FIG. 2). In contrast to the result with FluV, HS-058 inhibited strongly RSV infection in HeLa cells when it was added during the time of virus adsorption. HS-058 inhibited syncytium formation of HeLa cells by RSV infection. It appears that the antiviral mechanism of the polyoxometalate HS-058 occurs at two important points during virus-cell interactions. The first is adsorption of RSV to cell membrane and penetration (hemolysis) of FluV-A into cells. The second point is the late stage of virus infection by inhibiting cell-to-cell spread of RSV and FluV-A.

Of not was the recognition that several of the polyoxometalates which exhibited selective anti-HIV-1 activity were also potent antiviral agents against FluV-A (Table 2). This parity was not as strong with RSV or MLSV. HS-058 is a compound with modest anti-HIV-1 activity comparable to 2',3'-dideoxyinosine, a compound approved for the treatment of HIV.

The present invention also provides a method for treating human herpesvirus infection by administering a polyoxometalate. In the context of the present invention, the term human herpesvirus infection includes not only herpes simplex virus type 1 but also herpes simplex virus type 2 and cytomegalovirus. The present method specifically includes the treatment of herpes simplex virus type 1 (HSV-1), herpes simplex virus type 2 (HSV-2), cytomegalovirus (CMV), Epstein-Barr virus (EPV), human herpesvirus type 6 (HHV-6), human herpesvirus type 7 (HHV-7), and human herpesvirus type 8 (HHV-8). The preferred mode of administration for HSV-1, and HSV-2 is topical administration in the form of a cream containing 0.1 to 5% by weight, based on the total weight of the cream, of the polyoxometalate. In addition, the polyoxometalate may be administered systemically. For the other human herpesvirus infections, systemic administration is preferred, more preferably intravenous administration. The dosage range for the treatment of herpesvirus infection is the same as that used for the treatment of respiratory viral infection discussed above.

In another embodiment, the present invention provides a method for treating hepadnavirus infection, in particular hepatitis B virus (HBV), by administering a polyoxometalate. In this case, systemic administration is preferred, more preferably intravenous administration. Again, the dosage ranges for the treatment of hepadnavirus infection are the same as discussed above for the respiratory viral infection treatment.

In the case of treating herpes virus infection, and hepadnavirus infection, it is not only possible to use the polyoxometalate compounds discussed above, but in addition, it is possible to use the polyoxometalate compounds discussed in Ikeda et al, Antiviral Chemistry & Chemotherapy, vol. 4, pp. 253-262 (1993), which is incorporated herein by reference in its entirety.

Other features of the invention will become apparent in the course of the following descriptions of exemplary embodiments which are given for illustration of the invention and are not intended to be limiting thereof.

EXAMPLES Materials and Methods

Chemicals. Twenty five compounds were submitted to the antiviral assay (see Table 1 above) and synthesized according to the procedures which are published elsewhere. (Droege, M. W., et al, J. Mol. Catal., vol. 69, p. 323 (1991); Finke, R. G., et al, J. Am Chem. Soc., vol. 106, pp. 7274-7277 (1984); Finke, R. G., et al, Inorg. Chem., vol. 26, pp. 3886-3896 (1987); Hill, C. L., et al, J. Med. Chem., vol. 33, pp. 2767-2772 (1990); Hill, C. L., et al, in Advances in Chemotherapy of AIDS, Diasio, R. B. et al, Eds., Pergamon Press, New York, pp. 33-41 (1990); Kim, G.-S., et al, J. Med. Chem., vol. 37, pp. 816-820 (1994); Kim, G.-S., et al, unpublished work; Lyon, D. K., et al, J. Am. Chem. Soc., vol. 113, pp. 7209-7221 (1991), Weeks, M. S., et al, J. Med. Chem., vol. 35, pp. 1216-1221 (1992)). Dextran sulfates were purchased from Sigma Chemical Co. (St. Louis, Mo.).

Virus and cells. FluV, A/Ishikawa/7/82 (H3N2) and B/Sinagapore/222/79 had been passed more than 20 times in embryonated eggs. Both viruses were passed twice in Madin-Darby canine kidney (MDCK) cells before being used for virus growth or growth inhibition experiments in MDCK cells. RSV Long strain (type-A) had been passed in HEp-2 cells more than 20 times. Fresh isolates of RSV FM-58-8 (type-A) and SM-61-48 (type-B) were passed 5 times in HEp-2 cells after isolation. Measles virus (MLSV) Edmonston strain, mumps virus (MPSV) ECXH-3 strain, parainfluenzavirus (PFluV) type 2, Greer strain and (PFluV) type 3, C243 strain were passed 10 times in Vero cells, and MLSV, MPSV, and PFluV-2 were passed an additional 3 times in HMV-2 cells (Nishimura, H. K., et al, J. Gen. Virol., vol. 70, pp. 1653-1661 (1989)). Sources of virus strains and culture cell lines used for studies with the myxoviruses have been reported previously (Shigeta, S., et al, Antiviral Chem. Chemother., vol. 3, pp. 171-177 (1992); Shigeta, S., et al, Antimicrob. Agents Chemother., vol. 36, pp. 435-439 (1992).

MDCK, HEp-2, HMV-2 and Vero cells were cultured in Eagle's minimal essential medium (MEM) supplemented with 10% newborn calf serum, 100 units of penicillin G, and 100 mg of streptomycin per ml. For the infections of HEp-2 cells with RSV, HMV-2 cells with any of MLSV, MPSV and PFluV-2 and Vero cells with PFluV-3, a maintenance medium consisting of MEM with 2% heat=inactivated fetal calf serum and antibiotics was used. For the infection of MDCK cells with FluV, a maintenance medium consisting of MEM containing 0.2% bovine albumin, 2.5 μg/ml of crystallized trypsin (Sigma Chemical Co., St. Louis, Mo.) and antibiotics was used. For the plaque assay of RSV, HeLa cells grown in MEM supplemented with 10% newborn calf serum, 1.6% glucose and antibiotics, and MM consisting of MEM with 2% fetal calf serum, 1.6% glucose, antibiotics and 0.7% methyl cellulose (Methocel A-4M Premium; Dow Chemical Co. Midland Mich.) were used.

Antiviral assay. Antimyxovirus evaluation was principally followed the MTT assay by Pauwels et al. (Pauwels, R., et al, J. Virol. Meth., vol. 20, pp. 309-321 (1988). Four-fold dilution of compound (100 μl) was prepared in a 96 well tissue culture tray (Nunclon, 96 wells, Nunc A/S, Roskilde, Denmark) with 4 wells each for one dilution and combined with 10⁴ cells (50 μl) and 100 TCID₅₀ of virus (50 μl). The tray was centrifuged at 700 g for 5 minutes and incubated at 35° C. for 4 to 5 days. During the incubation, the culture medium with or without compound was changed after 3 days. To determine the median effective antiviral concentration (EC₅₀), we added 20 ml of 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide (MTT) at a concentration of 7 μg/ml in phosphate buffered saline (PBS, pH 7.2) to each well of cultures. The mixture was incubated at 37° C. for 2 hours and reduced MTT (formazan) was extracted by adding 100 μl of acidic isopropanol containing 4% Triton-X. The absorbance of blue color of formazan was measured using a computer controlled microplate reader (Model 3550, Bio Rad, Hercules, Calif.) at two different wavelengths (540 and 690 nm). The EC₅₀ was expressed as the concentration that achieved the 50% protection of virus infected cells from the virus induced destruction. The percent protection was calculated by the following formula:

    [(OD.sub.T)V-(OD.sub.C)V]/[(OD.sub.C)M-(OD.sub.C)V]×100(%),

where (OD_(T))V, (OD_(C))V and (OD_(C))M indicate the absorbance of the test sample, the virus infected control (no compound), and the mock infected control (no virus and no compound), respectively.

Antiviral activity against RSV was examined by a plaque reduction method. Monolayer cultures of HeLa cells were treated with 4-fold dilution of compound and infected with 50 plaque forming units (PFU) of virus. Virus and compound were diluted in maintenance media containing 0.7% methylcellulose. Infected cultures were incubated at 35° C. for 4 days, fixed with 5% formalin in PBS, stained with 0.02% crystal violet and the number of plaque in monolayer was counted under a microscope (40× magnification). The concentration of compound which reduced the number of plaques to 50% of the control was determined as the EC₅₀.

The anti-HIV-1 activity of the compounds was determined in human PBM cells as described previously (Schinazi, R. F., et al, Antimicrob. Agents Chemother., vol. 36, pp. 2423-2431 (1992)). Sterile stock solutions (40 mM) of the new compounds were prepared in water and then diluted to the desired concentration in medium. Cells were infected with the prototype HIV-1_(LA1) at a multiplicity of infection of 0.01. Virus obtained from the cell supernatant was quantitated on day 6 after infection by a reverse transcriptase assay using poly(rA)_(n) ·oligo(dT)₁₂₋₁₈ as template-primer. Studies have indicated a strong correlation (r² ≧0.88) between results obtained using the reverse transcriptase assay and a commercial HIV-1 p24 assay for polyoxometalates. The toxicity of the compounds was assessed in human PBM cells, as described previously (Schinazi, R. F., et al, Antimicrob. Agents Chemother., vol. 36, pp. 2423-2431 (1992)). The EC₅₀ and median inhibitory concentration (IC₅₀) were obtained from the concentration-response curve using the median effective method described by Chou and Talalay (Chou, T.-C., et al, Adv. Enzyme Regul., vol. 22, pp. 27-55 (1984)).

Immunofluorescent staining of RS virus infected cells. HeLa cells were seeded in Lab-Tek chamber slide (8 chambers, Nunc Inc.. Naperville, Ill.) and incubated at 37° C. in 5% CO₂. When the cell monolayer became confluent, approximately 50 PFU of RSV was inoculated in each well of the chamber. The cultures were incubated at 35° C. in a 5% CO₂ incubator. At 48 hours after infection, the maintenance media was removed, the cells were washed with PBS (pH, 7.2), and fixed with acetone for 10 minutes at room temperature. The fixed cells were stained with fluorescein isothiocyanate conjugated rabbit antibodies against RSV (Denka Seiken Co., Niigata, Japan) for 30 minutes at 37° C., mounted with 20% glycerol in PBS, and analyzed for immunofluorescence under a fluorescent microscope (Nikon Optiphot+EFD2, Nikon Industrial Co., Tokyo, Japan). Inhibitory effects of the compounds on RSV antigen synthesis and syncytium formation were monitored by counting the number of antigen positive foci or cells in a syncytium after immunofluorescent staining of infected cells. The details for the immunofluorescence for RSV were reported elsewhere (Shigeta, S., et al, Antiviral Chem. Chemother., vol. 3, pp. 171-177 (1992)).

Hemagglutination, hemolysis by influenzavirus, and inhibition assay. Fresh FluV-A was obtained from allantoic fluid of infected embryonated chicken egg. The virus was 2-fold diluted with PBS (pH 7.2), 100 μl distributed each to wells of a microtray, combined with the same volume of 0.5% fresh chicken erythrocytes, and was left at 4° C. for 1 hour. Titer of hemagglutinin (HA) of the virus was determined as 256 units/100 μl. After the hemagglutination, erythrocytes were centrifuged at 700 g for 5 minutes, resuspended in fresh 0.1 M sodium acetate buffer solution (pH, 5.25), and incubated at 37° C. for 30 minutes. The procedure reported by Huang et al (Huang, R. T. C., et al., Virology, vol. 110, pp. 243-247 (1981)) for hemolysis studies by FluV-A was followed. Maximum hemolysis was determined by absorbency at 540 nm which measures hemoglobin. For the inhibition of hemagglutination by the compounds, 2-fold dilutions of compound in PBS (pH 7.2) (100 μl), and 4 HA units of FluV-A (100 μl) were combined with 0.5% chick erythrocytes (200 μl), and the mixture was left at 4° C. for 1 hour. The minimal concentration of compounds which inhibited hemagglutination was determined as the minimal inhibitory dose (MID). For the inhibition of hemolysis, chick erythrocytes were agglutinated in several wells of a microtray by 100 units of HA following the procedure above. After hemagglutination, buffer was replaced with 2-fold dilution of compound in acetate buffer solution (pH 5.25), and the mixture was incubated at 37° C. for 30 minutes. The minimal concentration of compound which reduced the absorbance at 540 nm by 50% of control was defined as the EC₅₀.

RESULTS

Antiviral activities of several polyoxometalates against ortho- and paramyxoviruses. Twenty-five compounds (see Table 1 above) were evaluated for their inhibitory activities on the cytopathic effect of FluV-A, RSV and MLSV in tissue culture cells by MTT method. Among the compounds examined, 24 demonstrated antiviral activity against FluV-A, 11 showed activity against RSV, and 6 were effective against MLSV at lower concentrations than the cytotoxicity to each host cell (see Tables 2 and 3). Among the effective compounds. HS-054 or [Na₁₆ Fe₄ (H₂ O)₂ (P₂ W₁₅ O₅₆)₂ ·nH₂ O] (Wells-Dawson sandwich structure), HS-058 or [K₁₀ Fe₄ (H₂ O)₂ (PW₉ O₃₄)₂ ·nH₂ O] (Keggin sandwich structure), HS-106 or [(Me₃ NH)₈ Si₂ W₁₈ Nb₆ O₇₇ ·nH₂ O] (double Keggin structure), and HS-158 or (K₁₂ Nb₆ P₂ W₁₂ O₆₂) (hexasubstituted Wells-Dawson structure) exhibited potent and broad-spectrum antimyxovirus activities. These 4 compounds were further examined for antiviral activities against 9 myxovirus strains including an additional 6:FluV-B, MPSV, PFluV-2, PFluV-3, RSV-A, and RSV-B. Two RSV strains were fresh isolates from patients. The results shown in Table 3 indicate that FluV-A, FluV-B, RSV, MLSV, and PFluV-2 were susceptible to all 4 compounds at concentrations from 0.3 to 45.7 μM. On the other hand, MPSV and PFluV-3 were susceptible only to HS-054 at relatively high concentrations (21 to 28 μM). HS-058 showed EC₅₀ values of 1.4 μM against FluV-A, 13.9 μM against FluV-B, 5.6 μM against RSV (Long strain), 0.8 μM against MLSV and 0.43 μM against PFlu-V-2. HS-058 was not inhibitory for MPSV and PFluV-3 at 50 μM. HS-058 and HS-106 were less cytotoxic to MDCK and HEp-2 cells than HS-054 and HS-158, but more toxic to HMV-2 cells than the latter cell lines. HS-058 was not cytotoxic up to 200 μM for MDCK and HEp-2 cells, but had an IC₅₀ value of 50 μM for HMV-2 and Vero cells.

                                      TABLE 2                                      __________________________________________________________________________     ANTIVIRAL ACTIVITY OF POLYOXOMETALATES                                           FOR MYXOVIRUSES AND HIV-1 IN VITRO                                                 Antiviral activity, EC.sub.50 μM                                                            Cytotoxicity, IC.sub.50 μM                            Compound                                                                             FluV-A                                                                             RSV MLSV                                                                               HIV-1                                                                              MDCK                                                                               HEp-2                                                                              HMV-2                                                                              PBM                                          __________________________________________________________________________     HS-005                                                                               1.8.sup.a                                                                          1.9 1.5 0.4 50  1.9 26.0                                                                               35.0                                           HS-008 6.3   >50 >43 0.3   >100 50.0 43.0 >100.sup.                            HS-010 1.2   0.9   1.9   0.9 >100 12.4 30.0  1.8                               HS-026 0.23   >1.1 >3.7 0.3   16.0 1.1 3.9  7.7                                HS-042 2.7   >8.6 >16.2 4.7   >100 8.6 20.4 >100.sup.                          HS-052 0.9   >2.7 >0.8 0.1   >100 2.7 1.0 39.2                                 HS-053 1.1   1.4   >28.1 0.3   100 >50 25.6  4.5                               HS-054 0.7   1.4   0.2   0.4   >100 >50 >50 20.8                               HS-055 2.0   >26 >16 1.6   100 26.0 22.0 91.5                                  HS-056 21.1 >22 >1.6 4.5   50 22.0 1.8 93.1                                    HS-057 1.1   >50 20.6 1.3   100 >50 31.0 >100.sup.                             HS-058 1.1   3.8   0.76   1.7   >100 >50 50.0 >100.sup.                        HS-083 >35 >9.3 23.6 36.2   35.2 9.3 31.0 >100.sup.b                           HS-089 11.2 >3.7 >50 51.5 71.7 37.0 50.0 >100.sup.b                            HS-091 3.8   1.6 >80 0.2   50.0 6.2 8.0 .sup.  5.9.sup.b                       HS-105 5.0   4.5   >50 0.6   100 >50 >50 >100.sup.b                            HS-106 3.6   >9.3 >50 0.3   100 9.3 >50 >100.sup.b                             HS-131 2.5   9.2 >50 0.8   85.6 47.1 50.0 >100.sup.b                           HS-132 13.4   7.8 >50 0.8   >100 50.0 50.0 >100.sup.b                          HS-133 4.0   5.1   >10 1.4   100 >50 27.0 >100.sup.b                           HS-136 10.0   >50 >50 2.0   100 >50 >50 >100.sup.b                             HS-144 11.4   7.3   29 0.2   >100 >50 37.6 >100.sup.b                          HS-146 2.2   1.0 >4.5 0.2   56.6 8.0 12.8 .sup. 49.7.sup.b                     HS-157 2.1   11.6 >50 0.1   100 11.6 >50 .sup. 58.4.sup.b                      HS-158 1.5   >10 1.2   0.3   >100 10.0 44.2 .sup. 75.0.sup.b                   Ribavirin 8.7 4.7 5.2 NA >100 >50 >100 NA                                    __________________________________________________________________________      .sup.a Underline indicates that the effective antiviral concentration is       at least 10fold below the cytotoxic concentration. The variance for            duplicate or triplicate assays was less than 15%.                              .sup.b Cytotoxicity determined by .sup.3 Hthymidine uptake instead of cel      proliferation.                                                           

                                      TABLE 3                                      __________________________________________________________________________     INHIBITORY EFFECTS OF 4 POLYOXOMETALATES AGAINST                                 SEVERAL ORTHO- AND PARAMYXOVIRUSES                                                   EC.sub.50.sup.a and IC.sub.50 of Potyoxometalates, AM                  Virus strain                                                                           HS-054                                                                               HS-058                                                                               HS-106                                                                               HS-158                                                                               Ribavirin                                      __________________________________________________________________________     Antiviral Activity                                                               FluV-A 0.59 1.4 2.8 2.8 3.7                                                    (Ishikawa) (0.37-0.94) (0.7-2.0) (1.3-5.4) (1.0-5.5) (1.8-7.0)                 FluV-B 35.5 13.9 45.7 36.5 5.1                                                 (Singapore) (20-54) (8.7-21.8) (19.4-68) (30-43) (1.8-5.2)                     RSV-A 2.8 5.6 9.8 14.2 4.7                                                     (Long) (9.4-4.5) (2.4-13.5) (9.0-10.3) (8.3-24.4) (1.5-9.7)                    RSV-A 5.0.sup.b 23.0 10.0 8.5 3.5                                              (FM-58-8)                                                                      RSV-B 7.6.sup.b 3.1 4.5 2.7 1.6                                                (SM61-48)                                                                      MLSV 0.3 0.8 6.6 1.4 5.2                                                       (Edmonston) (0.2-0.4) (0.76-0.85) (5.6-7.6) (1.23-1.61) (1.9-10.0)                                            MPSV 20.6 >50 >50 >50 3.4                       (EXCH-3) (15.5-20) (3.1-37.1)                                                  PFluV-2 1.8 0.43 7.8 24.1 8.9                                                  (Greer) (1.5-2.1) (0.32-0.54) (2.6-16.1) (23.2-25.0) (6.4-11.2)                                               PFluV-3 28.0 >50 >50 >50 17.2                   (C243) (25-31)    (16.4-18.0)                                                  Cytotoxicity.sup.c                                                             MDCK >200 >200 >200 164 >200                                                    (>200).sup.c (>200) (200) (166) (>200)                                        HEp-2 88 >200 >200 82.7 52.7                                                    (38.0) (80.5) (192.2) (69.4) (>200)                                           HMV-2 >200 50 20.7 53.7 >100                                                    (94.1) (52.2) (70.7) (73.1) (>100)                                            Vero 50 50 148 >200 100                                                         (37.5) (38.4) (>200) (41.4) (>200)                                          __________________________________________________________________________      .sup.a Average of 3 to 4 independent experiments. Numbers in parentheses       show the range of values.                                                      .sup.b Data from one experiment.                                               .sup.c IC.sub.50 was examined by MTT method and viable cell counting. The      data in parentheses indicate the results of viable cell counting.        

Antiviral Effect of HS-058 Added Before, During, and After Virus Adsorption

In order to analyze the mechanism of antiviral activity of HS-058 against FluV-A and RSV, the compound was added to host cells before, during, and after virus infection. For the antiviral assay against FluV-A, MDCK cells were used and examined by MTT assay. For the assay against RSV, HeLa cells monolayers were used and examined by a plaque reduction method. As shown in Table 4, when HS-058 was added to the culture at 1 hour before the virus inoculation and maintained throughout the experiment, it was inhibitory against FluV-A at less than 0.7 μM and against RSV at 2.0 μM. When HS-058 was added to the culture 1 hour before and removed from the culture 1.5 hours after the virus inoculation, it was inhibitory against RSV at 2.4 μM, but was not inhibitory against FluV-A. When the compound was added after the virus adsorption (at 1.5 hour) and removed 3 hours after infection it was not inhibitory against both FluV-A and RSV. On the other hand, when the compound was added after virus adsorption and maintained throughout the experiment, it was inhibitory against both viruses at 4.1 and 5.8 μM (Table 4).

                  TABLE 4                                                          ______________________________________                                         TIME OF ADDITION AND INHIBITORY EFFECTS                                          OF HS-058 ON INFLUENZA AND RESPIRATORY                                         SYNCYTIAL VIRUS REPLICATIONS                                                     Time of addition                                                                              EC.sub.50 (μM) against:                                  of compound (hours).sup.a                                                                     FluV-A(Ishikawa)                                                                           RSV(Long)                                           ______________________________________                                         -1 to 120      0.7         2.0                                                   -1 to 1.5 >20 2.4                                                              1.5 to 120 4.1 5.8                                                             1.5 to 3 >31 >20                                                             ______________________________________                                          .sup.a Time of addition before or after virus inoculation. Cells were          washed extensively after removal of compound.                            

Inhibitory Effect of HS-054 and HS-058 Against Hemagglutination and Hemolysis of Chick Erythrocytes by Influenzavirus Type A

FluV-A binds to chick erythrocytes membrane at 4° C. in neutral buffered solution and hemolysis occurs at 37° C. in weakly acidic solution. The inhibitory effect of HS-054 and HS-058 against hemagglutination by 4 units of viral-HA and hemolysis by 100 units of viral-HA was examined. As shown in Table 5, both compounds did not inhibit hemagglutination at 100 μM, but inhibited hemolysis at 80 and 58 μM, respectively. On the other hand, dextran sulfates did not inhibit hemagglutation and hemolysis at all.

                  TABLE 5                                                          ______________________________________                                         INHIBITORY EFFECTS OF HS-058 FOR HEMAGGLUTINATION,                               HEMOLYSIS OF INFLUENZA VIRUS AND ANTIGEN SYNTHESIS,                            SYNCYTIUM FORMATION OF RESPIRATORY SYNCYTIAL VIRUS                                     Anti-FluV-A activity                                                                              Anti-RSV activity (μM)                           (μM) Inhibition for:  Inhibition for:                                     Compound  HA     Hemolysis   Antigen                                                                              Syncytium                                   ______________________________________                                         HS-054    >200   80(56-88).sup.a                                                                            >200.sup.                                                                            3.6(2.5-4.2)                                  HS-058 >200 58(350-81).sup.a >200.sup.  8.5(6.5-13)                            DS-8000.sup.b >200 >200.sup.c >200.sup.c >200.sup.c                            DS-50000.sup.b >200 >200.sup.  >200.sup.c >200.sup.c                         ______________________________________                                          .sup.a Average of 2 to 3 independent experiments. Numbers in parentheses       show range of value.                                                           .sup.b Molecular weights of dextran sulfates.                                  .sup.c Concentrations are expressed as μg/ml.                         

Inhibitory Effect of HS-054 and HS-058 Against Syncytium Formation by Respiratory Syncytial Virus

The inhibitory effect of HS-054 and HS-058 against syncytium formation of RSV in HeLa cell monolayers was examined by immunofluorescence. Both compounds inhibited syncytium formation of HeLa cells by RSV at 3.6 and 8.5 μM, respectively, but did not inhibit viral specific antigen synthesis at 100 μM (Table 5 and FIG. 2). Dextran sulfates did not inhibit antigen synthesis and syncytium formation at 100 μM.

Inhibitory Effect of HS-058 on One Step Growth of FluV-A in MDCK Cells

A 2-day culture of MDCK cells with confluent monolayer cells was prepared in 50 ml Nunclon tissue culture plates. Two sets of virus infected cultures were prepared. One set was infected with a high moi (5.0) and the other with a low moi (0.005). Both sets included virus control cultures which did not contain HS-058 throughout the experiment. Experimental cultures were treated with 4.4×EC₅₀ of the compound (6.0 μM) before (60 min) and after (90 min) virus inoculation while maintaining the compound throughout the culture period. Four to five flasks, prepared for each control and experimental cultures, were sampled at the time indicated in FIG. 1. The flasks were frozen at -80° C., thawed at 37° C., centrifuged at 700 g for 10 min and then titrated for yield of infectious virus in the supernatant. As shown in FIG. 1a, in the culture infected with high moi, HS-058 inhibited virus replication when added to cultures before virus adsorption, but was not inhibitory when added after virus adsorption to cells. In contrast, HS-058 inhibited virus yield production when the culture was infected with virus at a low moi, even when the compound was added after virus adsorption. These results indicate that the compound inhibits the virus adsorption and also cell-to-cell spread of virus.

Anti-HIV-1 Activity in Human Lymphocytes

Of the 25 compounds evaluated in acutely infected primary human PBM cells, 23 compounds demonstrated activity below 5 μM (Table 2). HS-008, HS-106, and HS-144 had a selectivity index greater than 300 and had no cytotoxicity to uninfected PBM cells when evaluated up to 100 μM. HS-058 was a modest inhibitor of HIV-1 with an EC₅₀ of 1.7 μM and no apparent cytotoxicity in any of the 4 different cells used.

Obviously, numerous modifications and variations of the present invention are possible in light of the above teachings. It is therefore to be understood that, within the scope of the appended claims, the invention may be practiced otherwise than as specifically described herein. 

What is claimed as new and desired to be secured by Letters Patent of the United States is:
 1. A method for preventing respiratory viral infection, comprising administering to a subject at risk an effective amount of a polyoxometalate selected from the group consisting of[(NMP)₂ H]₃ PW₁₂ O₄₀ [(DMA)₂ H]₃ PMo₁₂ O₄₀ (NH₄)₁₇ Na[NaSb₉ W₂₁ O₈₆ ] a- and b-H₅ BW₁₂ O₄₀ a- and b-H₆ ZnW₁₂ O₄₀ a- and b-H₆ P₂ W₁₈ O₆₂ α-(NH₄)₆ P₂ W₁₈ O₆₂ K₁₀ Cu₄ (H₂ O)₂ (PW₉ O₃₄)₂.20H₂ O K₁₀ Co₄ (H₂ O)₂ (PW₉ O₃₄)₂.20H₂ O Na₇ PW₁₁ O₃₉ Na₇ PW₁₁ O₃₉.20H₂ O+2C₆ H₅ P(O)(OH)₂ (n-Bu₄ N)₄ H₃ PW₁₁ O₃₉ b-Na₈ HPW₉ O₃₄ (n-Bu₄ N)₃ PMoW₁₁ O₃₉ a-[(nBu)₄ N]₄ Mo₈ O₂₆ (n-Bu₄ N)₂ W₆ O₁₉ (n-Bu₄ N)₂ Mo₆ O₁₉ a-(NH₄)_(n) H.sub.(4-n) SiW₁₂ O₄₀ a-(NH₄)_(n) H.sub.(5-n) BW₁₂ O₄₀ a-K₅ BW₁₂ O₄₀ K₄ W₄ O₁₀ (O₂)6 b-Na₉ HSiW₉ O₃₄ Na₆ H₂ W₁₂ O₄₀ (NH₄)₁₄ [NaP₅ W₃₀ O₁₁₀ ] a-(NH₄)₅ BW₁₂ O₄₀ a-Na₅ BW₁₂ O₄₀ (NH₄)₄ W₁₀ O₃₂ (Me₄ N)₄ W₁₀ O₃₂ (NISH⁺)_(n) H.sub.(5-n) BW₁₂ O₄₀ (LYSH⁺)_(n) H.sub.(5-n) BW₁₂ O40 (ARGH⁺)_(n) H.sub.(5-n) BW₁₂ O₄₀ (HISH⁺)_(n) H.sub.(4-n) SiW₁₂ O₄₀ (LYSH⁺)_(n) H.sub.(4-n) SiW₁₂ O₄₀ (ARGH⁺)_(n) H.sub.(4-n) SiW₁₂ O₄₀ a-K₈ SiW₁₁ O₃₉ a-K₈ SiW₁₁ O₃₉ K₁₀ (H₂ W₁₂ O₄₂) K₁₂ Ni₃ (II)(PW₉ O₃₄)₂.nH₂ O (NH₄)₁₀ Co₄ (II)(PW₉ O₃₄)₂.nH₂ O K₁₂ Pd₃ (II)(PW₉ O₃₄)₂.nH₂ O Na₁₂ P₂ W₁₅ O₅₆.18H₂ O Na₁₆ Cu₄ (H₂ O)₂ (P₂ W₁₅ O₅₆)₂.nH₂ O Na₁₆ Zn₄ (H₂ O)₂ (P₂ W₁₅ O₅₆)₂.nH₂ O Na₁₆ Co₄ (H₂ O)₂ (P₂ W₁₅ O₅₆)₂.nH₂ O Na₁₆ Ni₄ (H₂ O)₂ (P₂ W₁₅ O₅₆)₂.nH₂ O Na₁₆ Mn₄ (H₂ O)₂ (P₂ W₁₅ O₅₆).nH₂ O Na₁₆ Fe₄ (H₂ O)₂ (P₂ W₁₅ O₅₆)₂.nH₂ O K₁₀ Zn₄ (H₂ O)₂ (PW₉ O₃₄)₂.20H₂ O K₁₀ Ni₄ (H₂ O)₂ (PW₉ O₃₄)₂.nH₂ O K₁₀ Mn₄ (H₂ O)₂ (PW₉ O₃₄)₂.nH₂ O K₁₀ Fe₄ (H₂ O)₂ (PW₉ O₃₄)₂.nH₂ O K₁₂ Cu₃ (PW₉ O₃₄)₂.nH₂ O K₁₂ (Co H₂ O)₃ (PW₉ O₃₄)₂.nH₂ O K₁₂ Zn₃ (PW₉ O₃₄)₂.15H₂ O K₁₂ Mn₃ (PW₉ O₃₄)₂.15H₂ O K₁₂ Fe₃ (PW₉ O₃₄)₂.25H₂ O (ARGH⁺)₁₀ (NH₄)₇ Na[NaSb₉ W₂₁ O₈₆ ] (ARGH⁺)₅ HW₁₁ O₃₉.17H₂ O K₇ Ti₂ W₁₀ O₄₀ [(CH₃)₄ N]₇ Ti₂ W₁₀ O₄₀ Cs₇ Ti₂ W₁₀ O₄₀ [HISH+]₇ Ti₂ W₁₀ O₄₀ (LYSH+)_(n) Na_(7-n) PTi₂ W₁₀ O₄₀ (ARGH+)_(n) Na_(7-n) PTi₂ W₁₀ O₄₀ Cs₄ [SiW₁₁ O₃₉.O(SiCH₂ CH₂ C(O)OCH₃)₂ ]₄ -- [TBA]₃ H₃ V₁₀ O₂₈ K₇ HNb₆ O₁₉.13H₂ O K₈ Ta₆ O₁₉.17H₂ O [(CH₃)₄ N⁺ ]₄ SiW₁₁ O₃₉ --O(SiCH₂ CH₂ C(O)OCH₃)₂ [CH₃)₄ N⁺ ]₄ PW₁₁ O₃₉ --(SiCH₂ CH₂ CH₂ CN) [(CH₃)₄ N⁺ ]₄ PW₁₁ O₃₉ --(SiCH₂ CH₂ CH₂ Cl) [(CH₃)₄ N⁺ ]₄ PW₁₁ O₃₉ --(SiCH═CH₂) Cs₄ [SiW₁₁ O₃₉ --(SiCH₂ CH₂ CH₂ CN)₂ ] Cs₄ [SiW₁₁ O₃₉ --(SiCH₂ CH₂ CH₂ Cl)₂ ] Cs₄ [SiW₁₁ O₃₉ --(SiCH═CH₂)₂ ] [(CH₃)₄ N⁺ ]₄ SiW₁₁ O₃₉ O(SiCH₂ CH₂ CH₂ CH₂ CH₂ CH₃)₂ [(CH₃)₄ N⁺ ]₄ SiW₁₁ --O₃₉ O(SiCH₂ CH₂ CH₂ Cl)₂ [(CH₃)₄ N⁺ ]₄ SiW₁₁ O₃₉ --O(SiCH₂ CH₂ CH₂ CN)₂ [(CH₃)₄ N⁺ ]SiW₁₁ O₃₉ --O(SiCH═CH₂)₂ [(CH₂)₄ N⁺ ]SiW₁₁ O₃₉ --O(SiC(CH₃)₃)₂ [(CH₃)₄ N⁺ ]SiW₁₁ O₃₉ --O(SiCH₂ CH(CH₃)₂)₂ [(CH₃)₄ N⁺ ]₃ PW₁₁ O₃₉ O(SiCH₂ CH₂ COOCH₃)₂ K₅ Mn(II)PW₁₁ O₃₉ --nH₂ O K₈ Mn(II)P₂ W₁₇ O₆₁.nH₂ O K₆ Mn(II)SiW₁₁ O₃₉.nH₂ O K₅ PW₁₁ O₃₉ (SiMe₂).nH₂ O K₃ PW₁₁ O₄₁ (PPh)₂.xH₂ O Na₃ PW₁₁ O₄₁ (PPh)₂.xH₂ O K₅ PTiW₁₁ O₄₀ Cs₅ PTiW₁₁ O₃₉ K₆ SiW₁₁ O₃₉ (SiMe₂).nH₂ O K₃ PW₁₁ O₄₁ (PEt)₂.nH₂ O KSiW₁₁ O₃₉ [SiPh(t-Bu)].nH₂ O K₆ SiW₁₁ O₃₉ (SiPh₂).nH₂ O K₇ SiW₉ Nb₃ O₄₀.nH₂ O Cs₇ SiW₉ Nb₃ O₄₀.nH₂ O Cs₈ Si₂ W₁₈ Nb₆ O₇₇.nH₂ O (Me₃ NH)₇ SiW₉ Nb₃ O₄₀.nH₂ O (CH₃ H₆)₇ SiW₉ Nb₃ O₄₀.nH₂ O (CN₃ H₆)₈ Si₂ W₁₈ Nb₆ O₇₇.nH₂ O Rb₇ SiW₉ Nb₃ O₄₀.nH₂ O Rb₈ Si₂ W₁₈ Nb₆ O₇₇.nH₂ O K₈ Si₂ W₁₈ Nb₆ O₇₇.nH₂ O K₆ P₂ Mo₁₈ O₆₂.nH₂ O (C₅ H₅ N)₇ HSi₂ W₁₈ Nb₆ O₇₇.nH₂ O (C₅ H₅ N)₇ SiW₉ Nb₃ O₄₀.nH₂ O (ARGH⁺)₈ SiW₁₈ Nb₆ O₇₇.18H₂ O (LYSH⁺)₇ K SiW₁₈ Nb₆ O₇₇.18H₂ O (HISH⁺)₆ K₂ SiW₁₈ Nb₆ O₇₇.18H₂ O H₈ Si₂ W₁₈ Nb₆ O₇₇.nH₂ O (2 batches) [(CH₃)₄ N⁺ ]₄ SiW₁₁ O₃₉ --O(SiCH₂ CH₃)₂ [(CH₃)₄ N⁺ ]₄ SiW₁₁ O₃₉ --O(SiCH₃)₂ [(CH₃)₄ N⁺ ]₄ SiW₁₁ O₃₉ --O(SiC₁₆ H₃₃)₂ Li₇ HSi₂ W₁₈ Nb₆ O₇₇ Li₉ P₂ V₃ Me₃ W₁₂ O₆₂ Cs₉ P₂ V₃ MeW₁₂ O₆₂ Cs₁₂ P₂ V₃ W₁₂ O₆₂ K₄ H₂ PV₄ W₈ O₄₀ Na₁₂ P₄ W₁₄ O₅₈ Na₁₄ H₆ P₆ W₁₈ O₇₉ a-K₅ (NbO₂)SiW₁₁ O₃₉ K₅ (TaO₂)SiW₁₁ O₃₉ (Me₃ NH)₅ (NbO₂)SiW₁₁ O₃₉ (Me₃ NH)₅ NbSiW₁₁ O₄₀ (Me₃ NH)₅ (TaO₂)SiW₁₁ O₃₉ K₄ (NbO₂)PW₁₁ O₃₉ K₇ (NbO₂)P₂ W₁₂ O₆₁ (Me₃ NH)₇ (NbO₂)₃ SiW₉ O₃₇ Cs₇ (NbO₂)₃ SiW₉ O₃₇ K₆ (NbO₂)₃ PW₉ O₃₇ Na₁₀ (H₂ W₁₂ O₄₂) K₄ NbPW₁₁ O₄₀ (Me₃ NH)₄ NbPW₁₁ O₄₀ K₅ NbSiW₁₁ O₄₀ K₅ TaSiW₁₁ O₄₀ (Me₃ NH)₅ TaSiW₁₁ O₄₀ K₆ Nb₃ PW₉ O₄₀ K₇ NbP₂ W₁₇ O₆₂ K₇ (TiO₂)₂ PW₁₀ O₃₈ K₇ (TaO₂)₃ SiW₉ O₃₇ K₇ Ta₃ SiW₉ O₄₀ K₆ (TaO₂)₃ PW₉ O₃₇ K₆ Ta₃ PW₉ O₄₀ K₈ Co₂ W₁₁ O₃₉ H₂ (Me₄ N)₄ (EtSi)₂ CoW₁₁ O₄₀ H₂ (Me₄ N)₄ (iso-C₄ H₉ Si)₂ CoW₁₁ O₄₀ K₉ (NbO₂)₃ P₂ W₁₅ O₅₉ K₉ Nb₃ P₂ W₁₅ O₆₂ K₁₂ (NbO₂)₆ P₂ W₁₂ O₅₆ K₁₂ Nb₆ P₂ W₁₂ O₆₁ a₂ -K₁₀ P₂ W₁₇ O₆₁ K₆ Fe(III)Nb₃ P₂ W₁₅ O₆₂ K₇ Zn(II)Nb₃ P₂ W₁₅ O₆₂ (NH₄)₆ [a-P₂ W₁₈ O₆₂ ].nH₂ O K₁₂ [H₂ P₂ W₁₂ O₄₈ ].24H₂ O K₁₂ [H₂ P₂ W₁₂ O₄₈ ].24H₂ O K₂ Na₁.5 H₄.5 [PtMo₆ O₂₄ ].8H₂ O K₆ [a₂ -P₂ W₁₇ MoO₆₂ ].nH₂ O KHP₂ V₃ W₁₅ O₆₂.34H₂ O K₆ [P₂ W₁₂ Nb₆ O₆₂ ].24H₂ O Na₆ [V₁₀ O₂₈ ].18H₂ O (Guanidinium)₈ H[PV₁₄ O₆₂ ].3H₂ O K₈ H[PV₁₄ O₆₂ ] Na₇ [MnV₁₃ O₃₈ ].18H₂ O K₆ [BW₁₁ O₃₉ Ga(OH₂)].13H₂ O K₇ H[Nb₆ O₁₉ ].13H₂ O K₇ H[Nb₆ O₁₉ ].13H₂ O [MeN/Na/K]₄ [Nb₂ W₄ O₁₉ ] [Me₄ N]₉ [P₂ W₁₅ Nb₃ P₆₂ ] [Me₄ N]₁₅ [HP₄ W₃₀ Nb₆ O₁₂₃ ].16H₂ O [Me₄ N]₁₅ [HP₄ W₃₀ Nb₆ O₁₂₃ ].16H₂ O [Na/K]₆ Nb₄ W₂ O₁₉ ] [Me₄ N/Na/K]₅ [Nb₃ W₃ O₁₉ ].6H₂ O [Me₄ N/Na/K]₅ [Nb₃ W₃ O₁₉ ].6H₂ O [Me₅ CpRh)₄ V₆ O₁₉ ] K₅ [CpTiSiW₁₁ O₃₉ ].12H₂ O b₂ -K₈ [SiW₁₁ O₃₉ ].14H₂ O a-K₈ [SiW₁₀ O₃₆ ].12H₂ O Cs₇ Na₂ [PW₁₀ O₃₇ ].8H₂ O Cs₆ [P₂ W₅ O₂₃ ].7(1/2)H₂ O g-Cs₇ [PW₁₀ O₃₆ ].7H₂ O K₅ [SiNbW₁₁ O₄₀ ].7H₂ O K₄ [PNbW₁₁ O₄₀ ].12H₂ O Na₆ [Nb₄ W₂ O₁₉ ].13H₂ O Na₆ [Nb₄ W₂ O₁₉ ].20H₂ O K₆ [Nb₄ W₂ O₁₉ ].7H₂ O K₄ [V₂ W₄ O₁₉ ].3.5H₂ O Na₅ [V₃ W₃ O₁₉ ].12H₂ O K₆ [PV₃ W₉ O₄₀ ].14H₂ O Na₉ [A-b-GeW₉ O₃₄ ].8H₂ O Na₁₀ [A-a-GeW₉ O₃₄ ].9H₂ O K₇ [BV₂ W₁₀ O₄₀ ].6H₂ O Na₅ [CH₃ Sn(Nb₆ O₁₉)].10H₂ O Na₅ [CH₃ Sn(Nb₆ O₁₉)].10H₂ O Na₈ [Pt(P(m-SO₃ Ph)₃)₃ Cl].3H₂ O Na₃ [P(m-SO₃ Ph)₃ ].H₂ O (Me₃ NH)₁₀ (H)[Si₂ (ZrOH)₃ W₁₈ O₆₈ ].10H₂ O (Me₃ NH)₁₀ (H)[Si₂ (ZrOH)₃ W₁₈ O₆₈ ].10H₂ O K₇ [A-a-GeNb₃ W₉ O₄₀ ].18H₂ O K₇ [A-b-SiNb₃ W₉ O₄₀ ].20H₂ O (Me₃ NH)₉ [A-a-HSi₂ Nb₆ W₁₈ O₇₈ ] (Me₃ NH)₉ [A-a-HGe₂ Nb₆ W₁₈ O₇₈ ] (Me₃ NH)₉ [A-a-HGe₂ Nb₆ W₁₈ O₇₈ ] K₇ (H)[A-a-Ge₂ Nb₆ W₁₈ O₇₇ ].18H₂ O K₈ [A-b-Si₂ Nb₆ W₁₈ O₇₇ ] and (Me₃ NH)₈ [A-b-Si₂ Nb₆ W₁₈ O₇₇ ].
 2. The method of claim 1, wherein said polyoxometalate is selected from the group consisting of Na₁₇ P₇ W₁₅ O₅₆.18H₂ O, Na₁₆ Mn₄ (H₂ O)₂ (P₂ W₁₅ O₅₆).nH₂ O, K₁₀ Mn₄ (H₂ O)₂ (PW₉ O₃₄)₂.nH₂ O, K₁₀ Fe₄ (H₂ O)₂ (PW₉ O₃₄)₂.nH₂ O, (Me₃ NH)₇ SiW₉ NbO₄₀.nH₂ O, (Me₃ NH)₅ (NbO₂)SiW₁₁ O₃₉, H₂ (Me₄ N)₄ (EtSi)₂ CoW₁₁ O₄₀, and K₈ (A-β-Si₂ Nb₆ W₁₈ O₇₇).
 3. The method of claim 1, wherein said polyoxometalate is K₁₀ Fe₄ (H₂ O)₂ (PW₉ O₃₄)₂ n.H₂ O.
 4. The method of claim 1, wherein said respiratory viral infection is influenza A, influenza B, or RSV.
 5. The method of claim 1, wherein said polyoxometalate is administered in the form of an aerosol.
 6. The method of claim 1, wherein said polyoxometalate is K₈ (A-β-Si₂ Nb₆ W₁₈ O₇₇).
 7. A method for treating herpes virus infection, comprising administering to a patient in need thereof an effective amount of a polyoxometalate selected from the group consisting of[(NMP)₂ H]₃ PW₁₂ O₄₀ [(DMA)₂ H]₃ PMo₁₂ O₄₀ (NH₄)₁₇ Na[NaSb₉ W₂₁ O₈₆ ] a- and b-H₅ BW₁₂ O₄₀ a- and b-H₆ ZnW₁₂ O₄₀ a- and b-H₆ P₂ W₁₈ O₆₂ α-(NH₄)₆ P₂ W₁₈ O₆₂ K₁₀ Cu₄ (H₂ O)₂ (PW₉ O₃₄)₂.20H₂ O K₁₀ Co₄ (H₂ O)₂ (PW₉ O₃₄)₂.20H₂ O Na₇ PW₁₁ O₃₉ Na₇ PW₁₁ O₃₉.20H₂ O+2C₆ H₅ P(O)(OH)₂ (n-Bu₄ N)₄ H₃ PW₁₁ O₃₉ b-Na₈ HPW₉ O₃₄ (n-Bu₄ N)₃ PMoW₁₁ O₃₉ a-[(nBu)₄ N]₄ Mo₈ O₂₆ (n-Bu₄ N)₂ W₆ O₁₉ (n-Bu₄ N)₂ Mo₆ O₁₉ a-(NH₄)_(n) H.sub.(4-n) SiW₁₂ O₄₀ a-(NH₄)_(n) H.sub.(5-n) BW₁₂ O₄₀ a-K₅ BW₁₂ O₄₀ K₄ W₄ O₁₀ (O₂)6 b-Na₉ HSiW₉ O₃₄ Na₆ H₂ W₁₂ O₄₀ (NH₄)₁₄ [NaP₅ W₃₀ O₁₁₀ ] a-(NH₄)₅ BW₁₂ O₄₀ a-Na₅ BW₁₂ O₄₀ (NH₄)₄ W₁₀ O₃₂ (Me₄ N)₄ W₁₀ O₃₂ (HISH⁺)_(n) H.sub.(5-n) BW₁₂ O₄₀ (LYSH⁺)_(n) H.sub.(5-n) BW₁₂ O₄₀ (ARGH⁺)_(n) H.sub.(5-n) BW₁₂ O₄₀ (HISH⁺)_(n) H.sub.(4-n) SiW₁₂ O₄₀ (LYSH⁺)_(n) H.sub.(4-n) SiW₁₂ O₄₀ (ARGH⁺)_(n) H.sub.(4-n) SiW₁₂ O₄₀ a-K₈ SiW₁₁ O₃₉ a-K₈ SiW₁₁ O₃₉ K₁₀ (H₂ W₁₂ O₄₂) K₁₂ Ni₃ (II)(PW₉ O₃₄)₂.nH₂ O (NH₄)₁₀ Co₄ (II)(PW₉ O₃₄)₂.nH₂ O K₁₂ Pd₃ (II)(PW₉ O₃₄)₂.nH₂ O Na₁₂ P₂ W₁₅ O₅₆.18H₂ O Na₁₆ Cu₄ (H₂ O)₂ (P₂ W₁₅ O₅₆)₂.nH₂ O Na₁₆ Zn₄ (H₂ O)₂ (P₂ W₁₅ O₅₆)₂.nH₂ O Na₁₆ Co₄ (H₂ O)₂ (P₂ W₁₅ O₅₆)₂.nH₂ O Na₁₆ Ni₄ (H₂ O)₂ (P₂ W₁₅ O₅₆)₂.nH₂ O Na₁₆ Mn₄ (H₂ O)₂ (P₂ W₁₅ O₅₆).nH₂ O Na₁₆ Fe₄ (H₂ O)₂ (P₂ W₁₅ O₅₆)₂.nH₂ O K₁₀ Zn₄ (H₂ O)₂ (PW₉ O₃₄)₂.20H₂ O K₁₀ Ni₄ (H₂ O)₂ (PW₉ O₃₄)₂.nH₂ O K₁₀ Mn₄ (H₂ O)₂ (PW₉ O₃₄)₂.nH₂ O K₁₀ Fe₄ (H₂ O)₂ (PW₉ O₃₄)₂.nH₂ O K₁₂ Cu₃ (PW₉ O₃₄)₂.nH₂ O K₁₂ (Co H₂ O)₃ (PW₉ O₃₄)₂.nH₂ O K₁₂ Zn₃ (PW₉ O₃₄)₂.15H₂ O K₁₂ Mn₃ (PW₉ O₃₄)₂.15H₂ O K₁₂ Fe₃ (PW₉ O₃₄)₂.25H₂ O (ARGH⁺)₁₀ (NH₄)₇ Na[NaSb₉ W₂₁ O₈₆ ] (ARGH⁺)₅ HW₁₁ O₃₉.17H₂ O K₇ Ti₂ W₁₀ O₄₀ [(CH₃)₄ N]₇ Ti₂ W₁₀ O₄₀ Cs₇ Ti₂ W₁₀ O₄₀ [HISH+]₇ Ti₂ W₁₀ O₄₀ (LYSH+)_(n) Na_(7-n) PTi₂ W₁₀ O₄₀ (ARGH+)_(n) Na_(7-n) PTi₂ W₁₀ O₄₀ Cs₄ [SiW₁₁ O₃₉.O(SiCH₂ CH₂ C(O)OCH₃)₂ ]₄ -- [TBA]₃ H₃ V₁₀ O₂₈ K₇ HNb₆ O₁₉.13H₂ O K₈ Ta₆ O₁₉.17H₂ O [(CH₃)₄ N⁺ ]₄ SiW₁₁ O₃₉ --O(SiCH₂ CH₂ C(O)OCH₃)₂ [CH₃)₄ N⁺ ]₄ PW₁₁ O₃₉ --(SiCH₂ CH₂ CH₂ CN) [(CH₃)₄ N⁺ ]₄ PW₁₁ O₃₉ --(SiCH₂ CH₂ CH₂ Cl) [(CH₃)₄ N⁺ ]₄ PW₁₁ O₃₉ --(SiCH═CH₂) Cs₄ [SiW₁₁ O₃₉ --(SiCH₂ CH₂ CH₂ CN)₂ ] Cs₄ [SiW₁₁ O₃₉ --(SiCH₂ CH₂ CH₂ Cl)₂ ] Cs₄ [SiW₁₁ O₃₉ --(SiCH═CH₂)₂ ] [(CH₃)₄ N⁺ ]₄ SiW₁₁ O₃₉ O(SiCH₂ CH₂ CH₂ CH₂ CH₂ CH₃)₂ [(CH₃)₄ N⁺ ]₄ SiW₁₁ O₃₉ --O(SiCH₂ CH₂ CH₂ Cl)₂ [(CH₃)₄ N⁺ ]₄ SiW₁₁ O₃₉ --O(SiCH₂ CH₂ CH₃ CN)₂ [(CH₃)₄ N⁺ ]SiW₁₁ O₃₉ --O(SiCH═CH₂)₂ [(CH₂)₄ N⁺ ]SiW₁₁ O₃₉ --O(SiC(CH₃)₃)₂ [(CH₃)₄ N⁺ ]SiW₁₁ O₃₉ --O(SiCH₂ CH(CH₃)₂)₂ [(CH₃)₄ N⁺ ]₃ PW₁₁ O₃₉ O(SiCH₂ CH₂ COOCH₃)₂ K₅ Mn(II)PW₁₁ O₃₉ -nH₂ O K₈ Mn(II)P₂ W₁₇ O₆₁.nH₂ O K₆ Mn(II)SiW₁₁ O₃₉.nH₂ O K₅ PW₁₁ O₃₉ (SiMe₂).nH₂ O K₃ PW₁₁ O₄₁ (PPh)₂.xH₂ O Na₃ PW₁₁ O₄₁ (PPh)₂.xH₂ O K₅ PTiW₁₁ O₄₀ Cs₅ PTiW₁₁ O₃₉ K₆ SiW₁₁ O₃₉ (SiMe₂).nH₂ O K₃ PW₁₁ O₄₁ (PEt)₂.nH₂ O KSiW₁₁ O₃₉ [SiPh(t-Bu)].nH₂ O K₆ SiW₁₁ O₃₉ (SiPh₂).nH₂ O K₇ SiW₉ Nb₃ O₄₀.nH₂ O Cs₇ SiW₉ Nb₃ O₄₀.nH₂ O Cs₈ Si₂ W₁₈ Nb₆ O₇₇.nH₂ O (Me₃ NH)₇ SiW₉ Nb₃ O₄₀.nH₂ O (CN₃ H₆)₇ SiW₉ Nb₃ O₄₀.nH₂ O (CN₃ H₆)₈ Si₂ W₁₈ Nb₆ O₇₇.nH₂ O Rb₇ SiW₉ Nb₃ O₄₀.nH₂ O Rb₈ Si₂ W₁₈ Nb₆ O₇₇.nH₂ O K₈ Si₂ W₁₈ Nb₆ O₇₇.nH₂ O K₆ P₂ Mo₁₈ O₆₂.nH₂ O (C₅ H₅ N)₇ HSi₂ W₁₈ Nb₆ O₇₇.nH₂ O (C₅ H₅ N)₇ SiW₉ Nb₃ O₄₀.nH₂ (ARGH⁺)₈ SiW₁₈ Nb₆ O₇₇.18H₂ O (LYSH⁺)₇ K SiW₁₈ Nb₆ O₇₇.18H₂ O (HISH⁺)₆ K₂ SiW₁₈ Nb₆ O₇₇.18H₂ O H₈ Si₂ W₁₈ Nb₆ O₇₇.nH₂ O (2batches) [(CH₃)₄ N⁺ ]₄ SiW₁₁ O₃₉ --O(SiCH₂ CH₃)₂ [(CH₃)₄ N⁺ ]₄ SiW₁₁ O₃₉ --O(SiCH₃)₂ [(CH₃)₄ H⁺ ]₄ SiW₁₁ O₃₉ --O(SiC₁₆ H₃₃)₂ Li₇ HSi₂ W₁₈ Nb₆ O₇₇ Li₉ P₂ V₃ Me₃ W₁₂ O₆₂ Cs₉ P₂ V₃ MeW₁₂ O₆₂ Cs₁₂ P₂ V₃ W₁₂ O₆₂ K₄ H₂ PV₄ W₈ O₄₀ Na₁₂ P₄ W₁₄ O₅₈ Na₁₄ H₆ P₆ W₁₈ O₇₉ a-K₅ (NbO₂)SiW₁₁ O₃₉ K₅ (TaO₂)SiW₁₁ O₃₉ (Me₃ NH)₅ (NbO₂)SiW₁₁ O₃₉ (Me₃ NH)₅ NbSiW₁₁ O₄₀ (Me₃ NH)₅ (TaO₂)SiW₁₁ O₃₉ K₄ (NbO₂)PW₁₁ O₃₉ K₇ (NbO₂)P₂ W₁₂ O₆₁ (Me₃ NH)₇ (NbO₂)₃ SiW₉ O₃₇ Cs₇ (NbO₂)₃ SiW₉ O₃₇ K₆ (NbO₂)₃ PW₉ O₃₇ Na₁₀ (H₂ W₁₂ O₄₂) K₄ NbPW₁₁ O₄₀ (Me₃ NH)₄ NbPW₁₁ O₄₀ K₅ NbSiW₁₁ O₄₀ K₅ TaSiW₁₁ O₄₀ (Me₃ NH)₅ TaSiW₁₁ O₄₀ K₆ Nb₃ PW₉ O₄₀ K₇ NbP₂ W₁₇ O₆₂ K₇ (TiO₂)₂ PW₁₀ O₃₈ K₇ (TaO₂)₃ SiW₉ O₃₇ K₇ Ta₃ SiW₉ O₄₀ K₆ (TaO₂)₃ PW₉ O₃₇ K₆ Ta₃ PW₉ O₄₀ K₈ Co₂ W₁₁ O₃₉ H₂ (Me₄ N)₄ (EtSi)₂ CoW₁₁ O₄₀ H₂ (Me₄ N)₄ (iso-C₄ H₉ Si)₂ CoW₁₁ O₄₀ K₉ (NbO₂)₃ P₂ W₁₅ O₅₉ K₉ Nb₃ P₂ W₁₅ O₆₂ K₁₂ (NbO₂)₆ P₂ W₁₂ O₅₆ K₁₂ Nb₆ P₂ W₁₂ O₆₂ a₂ -K₁₀ P₂ W₁₇ O₆₁ K₆ Fe(III)Nb₃ P₂ W₁₅ O₆₂ K₇ Zn(II)Nb₃ P₂ W₁₅ O₆₂ (NH₄)₆ [a-P₂ W₁₈ O₆₂ ].nH₂ O K₁₂ [H₂ P₂ W₁₂ O₄₈ ].24H₂ O K₁₂ [H₂ P₂ W₁₂ O₄₈ ].24H₂ O K₂ Na₁.5 H₄.5 (PtMo₆ O₂₄ ].8H₂ O K₆ [a₂ -P₂ W₁₇ MoO₆₂ ].nH₂ O KHP₂ V₃ W₁₅ O₆₂.3H₂ O K₆ [P₂ W₁₂ Nb₆ O₆₂ ].24H₂ O Na₆ [V₁₀ O₂₈ ].18H₂ O (Guanidinium)₈ H[PV₁₄ O₆₂ ].3H₂ O K₈ H[PV₁₄ O₆₂ ] Na₇ [MnV₁₃ O₃₈ ].18H₂ O K₆ [BW₁₁ O₃₉ Ga(OH₂)].13H₂ O K₇ H[Nb₆ O₁₉ ].13H₂ O K₇ H[Nb₆ O₁₉ ].13H₂ O [MeN/Na/K]₄ [Nb₂ W₄ O₁₉ ] [Me₄ N]₉ [P₂ W₁₅ Nb₃ P₆₂ ] [Me₄ N]₁₅ [HP₄ W₃₀ Nb₆ O₁₂₃ ].16H₂ O [Me₄ N]₁₅ [HP₄ W₃₀ Nb₆ O₁₂₃ ].16H₂ O [Na/K]₆ Nb₄ W₂ O₁₉ ] [Me₄ N/Na/K]₅ [Nb₃ W₃ O₁₉ ].6H₂ O [Me₄ N/Na/K]₅ [Nb₃ W₃ O₁₉ ].6H₂ O [Me₅ CpRh)₄ V₆ O₁₉ ] K₅ [CpTiSiW₁₁ O₃₉ ].12H₂ O b₂ -K₈ [SiW₁₁ O₃₉ ].14H₂ O a-K₈ [SiW₁₀ O₃₆ ].12H₂ O Cs₇ Na₂ [PW₁₀ O₃₇ ].8H₂ O Cs₆ [P₂ W₅ O₂₃ ].7(1/2)H₂ O g-Cs₇ [PW₁₀ O₃₆ ].7H₂ O K₅ [SiNbW₁₁ O₄₀ ].7H₂ O K₄ [PNbW₁₁ O₄₀ ].12H₂ O Na₆ [Nb₄ W₂ O₁₉ ].13H₂ O Na₆ [Nb₄ W₂ O₁₉ ].20H₂ O K₆ [Nb₄ W₂ O₁₉ ].7H₂ O K₄ [V₂ W₄ O₁₉ ].3.5H₂ O Na₅ [V₃ W₃ O₁₉ ].12H₂ O K₆ [PV₃ W₉ O₄₀ ].14H₂ O Na₉ [A-b-GeW₉ O₃₄ ].8H₂ O Na₁₀ [A-a-GeW₉ O₃₄ ].9H₂ O K₇ [BV₂ W₁₀ O₄₀ ].6H₂ O Na₅ [CH₃ Sn(Nb₆ O₁₉)].10H₂ O Na₅ [CH₃ Sn(Nb₆ O₁₉)].10H₂ O Na₈ [Pt(P(m-SO₃ Ph)₃)₃ Cl].3H₂ O Na₃ [P(m-SO₃ Ph)₃ ].H₂ O (Me₃ NH)₁₀ (H)[Si₂ (ZrOH)₃ W₁₈ O₆₈ ].10H₂ O (Me₃ NH)₁₀ (H)[Si₂ (ZrOH)₃ W₁₈ O₆₈ ].10H₂ O K₇ [A-a-GeNb₃ W₉ O₄₀ ].18H₂ O K₇ [A-b-SiNb₃ W₉ O₄₀ ].20H₂ O (Me₃ NH)₉ [A-a-HSi₂ Nb₆ W₁₈ O₇₈ ] (Me₃ NH)₉ [A-a-HGe₂ Nb₆ W₁₈ O₇₈ ] (Me₃ NH)₉ [A-a-HGe₂ Nb₆ W₁₈ O₇₈ ] K₇ (H)[A-a-Ge₂ Nb₆ W₁₈ O₇₇ ].18H₂ O K₈ [A-b-Si₂ Nb₆ W₁₈ O₇₇ ] and (Me₃ NH)₈ [A-b-Si₂ Nb₆ W₁₈ O₇₇ ].
 8. The method of claim 7, wherein said herpesvirus is selected from the group consisting of herpes simplex virus type 1, herpes simplex virus type 2, cytomegalovirus, Epstein-Barr virus, human herpesvirus type 6, human herpesvirus type 7, and human herpesvirus type
 8. 9. The method of claim 7, wherein said polyoxometalate is K₈ (A-β-Si₂ Nb₆ W₁₈ O₇₇).
 10. A method for treating hepadnavirus infection, comprising administering to a patient in need thereof an effective amount of a polyoxometalate selected from the group consisting of[(NMP)₂ H]₃ PW₁₂ O₄₀ [(DMA)₂ H]₃ PMo₁₂ O₄₀ (NH₄)₁₇ Na[NaSb₉ W₂₁ O₈₆ ] a- and b-H₅ BW₁₂ O₄₀ a- and b-H₆ ZnW₁₂ O₄₀ a- and b-H₆ P₂ W₁₈ O₆₂ α-(NH₄)₆ P₂ W₁₈ O₆₂ K₁₀ Cu₄ (H₂ O)₂ (PW₉ O₃₄)₂.20H₂ O K₁₀ Co₄ (H₂ O)₂ (PW₉ O₃₄)₂.20H₂ O Na₇ PW₁₁ O₃₉ Na₇ PW₁₁ O₃₉.20H₂ O+2C₆ H₅ P(O)(OH)₂ (n-Bu₄ N)₄ H₃ PW₁₁ O₃₉ b-Na₈ HPW₉ O₃₄ (n-Bu₄ N)₃ PMoW₁₁ O₃₉ a-[(nBu)₄ N]₄ Mo₈ O₂₆ (n-Bu₄ N)₂ W₆ O₁₉ (n-Bu₄ N)₂ Mo₆ O₁₉ a-(NH₄)_(n) H.sub.(4-n) SiW₁₂ O₄₀ a-(NH₄)_(n) H.sub.(5-n) BW₁₂ O₄₀ a-K₅ BW₁₂ O₄₀ K₄ W₄ O₁₀ (O₂)6 b-Na₉ HSiW₉ O₃₄ Na₆ H₂ W₁₂ O₄₀ (NH₄)₁₄ [NaP₅ W₃₀ O₁₁₀ ] a-(NH₄)₅ BW₁₂ O₄₀ a-Na₅ BW₁₂ O₄₀ (NH₄)₄ W₁₀ O₃₂ (Me₄ N)₄ W₁₀ O₃₂ (HISH⁺)_(n) H.sub.(5-n) BW₁₂ O₄₀ (LYSH⁺)_(n) H.sub.(5-n) BW₁₂ O₄₀ (ARGH⁺)_(n) H.sub.(5-n) BW₁₂ O₄₀ (HISH⁺)_(n) H.sub.(4-n) SiW₁₂ O₄₀ (LYSH⁺)_(n) H.sub.(4-n) SiW₁₂ O₄₀ (ARGH⁺)_(n) H.sub.(4-n) SiW₁₂ O₄₀ a-K₈ SiW₁₁ O₃₉ a-K₈ SiW₁₁ O₃₉ K₁₀ (H₂ W₁₂ O₄₂) K₁₂ Ni₃ (II)(PW₉ O₃₄)₂.nH₂ O (NH₄)₁₀ Co₄ (II)(PW₉ O₃₄)₂.nH₂ O K₁₂ Pd₃ (II)(PW₉ O₃₄)₂.nH₂ O Na₁₂ P₂ W₁₅ O₅₆.18H₂ O Na₁₆ Cu₄ (H₂ O)₂ (P₂ W₁₅ O₅₆)₂.nH₂ O Na₁₆ Zn₄ (H₂ O)₂ (P₂ W₁₅ O₅₆)₂.nH₂ O Na₁₆ Co₄ (H₂ O)₂ (P₂ W₁₅ O₅₆)₂.nH₂ O Na₁₆ Ni₄ (H₂ O)₂ (P₂ W₁₅ O₅₆)₂.nH₂ O Na₁₆ Mn₄ (H₂ O)₂ (P₂ W₁₅ O₅₆)nH₂ O Na₁₆ Fe₄ (H₂ O)₂ (P₂ W₁₅ O₅₆)₂.nH₂ O K₁₀ Zn₄ (H₂ O)₂ (PW₉ O₃₄)₂.20H₂ O K₁₀ Ni₄ (H₂ O)₂ (PW₉ O₃₄)₂.nH₂ O K₁₀ Mn₄ (H₂ O)₂ (PW₉ O₃₄)₂.nH₂ O K₁₀ Fe₄ (H₂ O)₂ (PW₉ O₃₄)₂.nH₂ O K₁₂ Cu₃ (PW₉ O₃₄)₂.nH₂ O K₁₂ (Co H₂ O)₃ (PW₉ O₃₄)₂.nH₂ O K₁₂ Zn₃ (PW₉ O₃₄)₂.15H₂ O K₁₂ Mn₃ (PW₉ O₃₄)₂.15H₂ O K₁₂ Fe₃ (PW₉ O₃₄)₂.25H₂ O (ARGH⁺)₁₀ (NH₄)₇ Na[NaSb₉ W₂₁ O₈₆ ] (ARGH⁺)₅ HW₁₁ O₃₉.17H₂ O K₇ Ti₂ W₁₀ O₄₀ [(CH₃)₄ N]₇ Ti₂ W₁₀ O₄₀ Cs₇ Ti₂ W₁₀ O₄₀ [HISH+]₇ Ti₂ W₁₀ O₄₀ (LYSH+)_(n) Na_(7-n) PTi₂ W₁₀ O₄₀ (ARGH+)_(n) Na_(7-n) PTi₂ W₁₀ O₄₀ Cs₄ [SiW₁₁ O₃₉.O(SiCH₂ CH₂ C(O)OCH₃)₂ ]₄ -- [TBA]₃ H₃ V₁₀ O₂₈ K₇ HNb₆ O₁₉.13H₂ O K₈ Ta₆ O₁₉.17H₂ O [(CH₃)₄ N⁺ ]₄ SiW₁₁ O₃₉ --O(SiCH₂ CH₂ C(O)OCH₃)₂ [CH₃)₄ N⁺ ]₄ PW₁₁ O₃₉ --(SiCH₂ CH₂ CH₂ CN) [(CH₃)₄ N⁺ ]₄ PW₁₁ O₃₉ --(SiCH₂ CH₂ CH₂ Cl) [(CH₃)₄ N⁺ ]₄ PW₁₁ O₃₉ --(SiCH═CH₂) Cs₄ [SiW₁₁ O₃₉ --(SiCH₂ CH₂ CH₂ CN)₂ ] Cs₄ [SiW₁₁ O₃₉ --(SiCH₂ CH₂ CH₂ Cl)₂ ] Cs₄ [SiW₁₁ O₃₉ --(SiCH═CH₂)₂ ] [(CH₃)₄ N⁺ ]₄ SiW₁₁ O₃₉ O(SiCH₂ CH₂ CH₂ CH₂ CH₂ CH₃)₂ [(CH₃)₄ N⁺ ]₄ SiW₁₁ O₃₉ --O(SiCH₂ CH₂ CH₂ Cl)₂ [(CH₃)₄ N⁺ ]₄ SiW₁₁ O₃₉ --O(SiCH₂ CH₂ CH₂ CN)₂ [(CH₃)₄ N⁺ ]SiW₁₁ O₃₉ --O(SiCH═CH₂)₂ [(CH₂)₄ N⁺ ]SiW₁₁ O₃₉ --O(SiC(CH₃)₃)₂ [(CH₃)₄ N⁺ ]SiW₁₁ O₃₉ --O(SiCH₂ CH(CH₃)₂)₂ [(CH₃)₄ N⁺ PW₁₁ O₃₉ O(SiCH₂ CH₂ COOCH₃)₂ K₅ Mn(II)PW₁₁ O₃₉ -nH₂ O K₈ Mn(II)P₂ W₁₇ O₆₁.nH₂ O K₆ Mn(II)SiW₁₁ O₃₉.nH₂ O K₅ PW₁₁ O₃₉ (SiMe₂).nH₂ O K₃ PW₁₁ O₄₁ (PPh)₂.xH₂ O Na₃ PW₁₁ O₄₁ (PPh)₂.xH₂ O K₅ PTiW₁₁ O₄₀ Cs₅ PTiW₁₁ O₃₉ K₆ SiW₁₁ O₃₉ (SiMe₂).nH₂ O K₃ PW₁₁ O₄₁ (PEt)₂.nH₂ O KSiW₁₁ O₃₉ [SiPh(t-Bu)].nH₂ O K₆ SiW₁₁ O₃₉ (SiPh₂).nH₂ O K₇ SiW₉ Nb₃ O₄₀.nH₂ O Cs₇ SiW₉ Nb₃ O₄₀.nH₂ O Cs₈ Si₂ W₁₈ Nb₆ O₇₇.nH₂ O (Me₃ NH)₇ SiW₉ Nb₃ O₄₀.nH₂ O (CN₃ H₆)₇ SiW₉ Nb₃ O₄₀.nH₂ O (CN₃ H₆)₈ Si₂ W₁₈ Nb₆ O₇₇.nH₂ O Rb₇ SiW₉ Nb₃ O₄₀.nH₂ O Rb₈ Si₂ W₁₈ Nb₆ O₇₇.nH₂ O K₈ Si₂ W₁₈ Nb₆ O₇₇.nH₂ O K₆ P₂ Mo₁₈ O₆₂.nH₂ O (C₅ H₅ N)₇ HSi₂ W₁₈ Nb₆ O₇₇.nH₂ O (C₅ H₅ N)₇ SiW₉ Nb₃ O₄₀.nH₂ O (ARGH⁺)₈ SiW₁₈ Nb₆ O₇₇.18H₂ O (LYSH⁺)₇ K SiW₁₈ Nb₆ O₇₇.18H₂ O (HISH⁺)₆ K₂ SiW₁₈ Nb₆ O₇₇.18H₂ O H₈ Si₂ W₁₈ Nb₆ O₇₇.nH₂ O (2 batches) [(CH₃)₄ N⁺ ]₄ SiW₁₁ O₃₉ --O(SiCH₂ CH₃)₂ [(CH₃)₄ N⁺ ]₄ SiW₁₁ O₃₉ --O(SiCH₃)₂ [(CH₃)₄ N⁺ ]₄ SiW₁₁ O₃₉ --O(SiC₁₆ H₃₃)₂ Li₇ HSi₂ W₁₈ Nb₆ O₇₇ Li₉ P₂ V₃ Me₃ W₁₂ O₆₂ Cs₉ P₂ V₃ MeW₁₂ O₆₂ Cs₁₂ P₂ V₃ W₁₂ O₆₂ K₄ H₂ PV₄ W₈ O₄₀ Na₁₂ P₄ W₁₄ O₅₈ Na₁₄ H₆ P₆ W₁₈ O₇₉ a-K₅ (Nb_(O) ₂)SiW₁₁ O₃₉ K₅ (TaO₂)SiW₁₁ O₃₉ (Me₃ NH)₅ (NbO₂)SiW₁₁ O₃₉ (Me₃ NH)₅ NbSiW₁₁ O₄₀ (Me₃ NH)₅ (TaO₂)SiW₁₁ O₃₉ K₄ (NbO₂)PW₁₁ O₃₉ K₇ (NbO₂)P₂ W₁₂ O₆₁ (Me₃ NH)₇ (NbO₂)₃ SiW₉ O₃₇ Cs₇ (NbO₂)₃ SiW₉ O₃₇ K₆ (NbO₂)₃ PW₉ O₃₇ Na₁₀ (H₂ W₁₂ O₄₂) K₄ NbPW₁₁ O₄₀ (Me₃ NH)₄ NbPW₁₁ O₄₀ K₅ NbSiW₁₁ O₄₀ K₅ TaSiW₁₁ O₄₀ (Me₃ NH)₅ TaSiW₁₁ O₄₀ K₆ Nb₃ PW₉ O₄₀ K₇ NbP₂ W₁₇ O₆₂ K₇ (TiO₂)₂ PW₁₀ O₃₈ K₇ (TaO₂)₃ SiW₉ O₃₇ K₇ Ta₃ SiW₉ O₄₀ K₆ (TaO₂)₃ PW₉ O₃₇ K₆ Ta₃ PW₉ O₄₀ K₈ Co₂ W₁₁ O₃₉ H₂ (Me₄ N)₄ (EtSi)₂ CoW₁₁ O₄₀ H₂ (Me₄ N)₄ (iso-C₄ H₉ Si)₂ CoW₁₁ O₄₀ K₉ (NbO₂)₃ P₂ W₁₅ O₅₉ K₉ Nb₃ P₂ W₁₅ O₆₂ K₁₂ (NbO₂)₆ P₂ W₁₂ O₅₆ K₁₂ Nb₆ P₂ W₁₂ O₆₂ a₂ -K₁₀ P₂ W₁₇ O₆₁ K₆ Fe(III)Nb₃ P₂ W₁₅ O₆₂ K₇ Zn(II)Nb₃ P₂ W₁₅ O₆₂ (NH₄)₆ [a-P₂ W₁₈ O₆₂ ].nH₂ O K₁₂ [H₂ P₂ W₁₂ O₄₈ ].24H₂ O K₁₂ [H₂ P₂ W₁₂ O₄₈ ].24H₂ O K₂ Na₁.5 H₄.5 [PtMo₆ O₂₄ ].8H₂ O K₆ [a₂ -P₂ W₁₇ MoO₆₂ ].nH₂ O KHP₂ V₃ W₁₅ O₆₂.34H₂ O K₆ [P₂ W₁₂ Nb₆ O₆₂ ].24H₂ O Na₆ [V₁₀ O₂₈ ].18H₂ O (Guanidinium)₈ H[PV₁₄ O₆₂ ].3H₂ O K₈ H[PV₁₄ O₆₂ ] Na₇ [MnV₁₃ O₃₈ ].18H₂ O K₆ [BW₁₁ O₃₉ Ga(OH₂)].13H₂ O K₇ H[Nb₆ O₁₉ ].13H₂ O K₇ H[Nb₆ O₁₉ ].13H₂ O [MeN/Na/K]₄ [Nb₂ W₄ O₁₉ ] [Me₄ N]₉ [P₂ W₁₅ Nb₃ P₆₂ ] [Me₄ N]₁₅ [HP₄ W₃₀ Nb₆ O₁₂₃ ].16H₂ O [Me₄ N]₁₅ [HP₄ W₃₀ Nb₆ O₁₂₃ ].16H₂ O [Na/K]₆ Nb₄ W₂ O₁₉ ] [Me₄ N/Na/K]₅ [Nb₃ W₃ O₁₉ ].6H₂ O [Me₄ N/Na/K]₅ [Nb₃ W₃ O₁₉ ].6H₂ O [Me₅ CpRh)₄ V₆ O₁₉ ] K₅ [CpTiSiW₁₁ O₃₉ ].12H₂ O b₂ -K₈ [SiW₁₁ O₃₉ ].14H₂ O a-K₈ [SiW₁₀ O₃₆ ].12H₂ O Cs₇ Na₂ [PW₁₀ O₃₇ ].8H₂ O Cs₆ [P₂ W₅ O₂₃ ].7(1/2)H₂ O g-Cs₇ [PW₁₀ O₃₆ ].7H₂ O K₅ [SiNbW₁₁ O₄₀ ].7H₂ O K₄ [PNbW₁₁ O₄₀ ].12H₂ O Na₆ [Nb₄ W₂ O₁₉ ].13H₂ O Na₆ [Nb₄ W₂ O₁₉ ].20H₂ O K₆ [Nb₄ W₂ O₁₉ ].7H₂ O K₄ [V₂ W₄ O₁₉ ].3.5H₂ O Na₅ [V₃ W₃ O₁₉ ].12H₂ O K₆ [PV₃ W₉ O₄₀ ].14H₂ O Na₉ [A-b-GeW₉ O₃₄ ].8H₂ O Na₁₀ [A-a-GeW₉ O₃₄ ].9H₂ O K₇ [BV₂ W₁₀ O₄₀ ].6H₂ O Na₅ [CH₃ Sn(Nb₆ O₁₉)].10H₂ O Na₅ [CH₃ Sn(Nb₆ O₁₉)].10H₂ O Na₈ [Pt(P(m-SO₃ Ph)₃)₃ Cl].3H₂ O Na₃ [P(m-SO₃ Ph)₃ ].H₂ O (Me₃ NH)₁₀ (H)[Si₂ (ZrOH)₃ W₁₈ O₆₈ ].10H₂ O (Me₃ NH)₁₀ (H)[Si₂ (ZrOH)₃ W₁₈ O₆₈ ].10H₂ O K₇ [A-a-GeNb₃ W₉ O₄₀ ].18H₂ O K₇ [A-b-SiNb₃ W₉ O₄₀ ].20H₂ O (Me₃ NH)₉ [A-a-HSi₂ Nb₆ W₁₈ O₇₈ ] (Me₃ NH)₉ [A-a-HGe₂ Nb₆ W₁₈ O₇₈ ] (Me₃ NH)₉ [A-a-HGe₂ Nb₆ W₁₈ O₇₈ ] K₇ (H)[A-a-Ge₂ Nb₆ W₁₈ O₇₇ ].18H₂ O K₈ [A-b-Si₂ Nb₆ W₁₈ O₇₇ ] and (Me₃ NH)₈ [A-b-Si₂ Nb₆ W₁₈ O₇₇ ].
 11. The method of claim 10, wherein said hepadnavirus is hepatitis B virus.
 12. The method of claim 10, wherein said polyoxometalate is K₈ (A-β-Si₂ Nb₆ W₁₈ O₇₇). 